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Population genetics

January 10, 2023

Population genetics is a subfield of genetics that deals with genetic differences within and between populations, and is a part of evolutionary biology. Studies in this branch of biology examine such phenomena as adaptation, speciation, and population structure.[1]

Population genetics was a vital ingredient in the emergence of the modern evolutionary synthesis. Its primary founders were Sewall Wright, J. B. S. Haldane and Ronald Fisher, who also laid the foundations for the related discipline of quantitative genetics. Traditionally a highly mathematical discipline, modern population genetics encompasses theoretical, laboratory, and field work. Population genetic models are used both for statistical inference from DNA sequence data and for proof/disproof of concept.[2]

What sets population genetics apart from newer, more phenotypic approaches to modelling evolution, such as evolutionary game theory and adaptive dynamics, is its emphasis on such genetic phenomena as dominance, epistasis, the degree to which genetic recombination breaks linkage disequilibrium, and the random phenomena of mutation and genetic drift. This makes it appropriate for comparison to population genomics data.

History

Population genetics began as a reconciliation of Mendelian inheritance and biostatistics models. Natural selection will only cause evolution if there is enough genetic variation in a population. Before the discovery of Mendelian genetics, one common hypothesis was blending inheritance. But with blending inheritance, genetic variance would be rapidly lost, making evolution by natural or sexual selection implausible. The Hardy–Weinberg principle provides the solution to how variation is maintained in a population with Mendelian inheritance. According to this principle, the frequencies of alleles (variations in a gene) will remain constant in the absence of selection, mutation, migration and genetic drift.[3]

 
The typical white-bodied form of the peppered moth.
 
Industrial melanism: the black-bodied form of the peppered moth appeared in polluted areas.

The next key step was the work of the British biologist and statistician Ronald Fisher. In a series of papers starting in 1918 and culminating in his 1930 book The Genetical Theory of Natural Selection, Fisher showed that the continuous variation measured by the biometricians could be produced by the combined action of many discrete genes, and that natural selection could change allele frequencies in a population, resulting in evolution. In a series of papers beginning in 1924, another British geneticist, J. B. S. Haldane, worked out the mathematics of allele frequency change at a single gene locus under a broad range of conditions. Haldane also applied statistical analysis to real-world examples of natural selection, such as peppered moth evolution and industrial melanism, and showed that selection coefficients could be larger than Fisher assumed, leading to more rapid adaptive evolution as a camouflage strategy following increased pollution.[4][5]

The American biologist Sewall Wright, who had a background in animal breeding experiments, focused on combinations of interacting genes, and the effects of inbreeding on small, relatively isolated populations that exhibited genetic drift. In 1932 Wright introduced the concept of an adaptive landscape and argued that genetic drift and inbreeding could drive a small, isolated sub-population away from an adaptive peak, allowing natural selection to drive it towards different adaptive peaks.[citation needed]

The work of Fisher, Haldane and Wright founded the discipline of population genetics. This integrated natural selection with Mendelian genetics, which was the critical first step in developing a unified theory of how evolution worked.[4][5] John Maynard Smith was Haldane's pupil, whilst W. D. Hamilton was influenced by the writings of Fisher. The American George R. Price worked with both Hamilton and Maynard Smith. American Richard Lewontin and Japanese Motoo Kimura were influenced by Wright and Haldane.[citation needed]

Modern synthesis

Main article: Modern synthesis (20th century)

The mathematics of population genetics were originally developed as the beginning of the modern synthesis. Authors such as Beatty[6] have asserted that population genetics defines the core of the modern synthesis. For the first few decades of the 20th century, most field naturalists continued to believe that Lamarckism and orthogenesis provided the best explanation for the complexity they observed in the living world.[7] During the modern synthesis, these ideas were purged, and only evolutionary causes that could be expressed in the mathematical framework of population genetics were retained.[8] Consensus was reached as to which evolutionary factors might influence evolution, but not as to the relative importance of the various factors.[8]

Theodosius Dobzhansky, a postdoctoral worker in T. H. Morgan's lab, had been influenced by the work on genetic diversity by Russian geneticists such as Sergei Chetverikov. He helped to bridge the divide between the foundations of microevolution developed by the population geneticists and the patterns of macroevolution observed by field biologists, with his 1937 book Genetics and the Origin of Species. Dobzhansky examined the genetic diversity of wild populations and showed that, contrary to the assumptions of the population geneticists, these populations had large amounts of genetic diversity, with marked differences between sub-populations. The book also took the highly mathematical work of the population geneticists and put it into a more accessible form. Many more biologists were influenced by population genetics via Dobzhansky than were able to read the highly mathematical works in the original.[9]

In Great Britain E. B. Ford, the pioneer of ecological genetics,[10] continued throughout the 1930s and 1940s to empirically demonstrate the power of selection due to ecological factors including the ability to maintain genetic diversity through genetic polymorphisms such as human blood types. Ford's work, in collaboration with Fisher, contributed to a shift in emphasis during the modern synthesis towards natural selection as the dominant force.[4][5][11][12]

Neutral theory and origin-fixation dynamics

The original, modern synthesis view of population genetics assumes that mutations provide ample raw material, and focuses only on the change in frequency of alleles within populations.[13] The main processes influencing allele frequencies are natural selection, genetic drift, gene flow and recurrent mutation. Fisher and Wright had some fundamental disagreements about the relative roles of selection and drift.[14] The availability of molecular data on all genetic differences led to the neutral theory of molecular evolution. In this view, many mutations are deleterious and so never observed, and most of the remainder are neutral, i.e. are not under selection. With the fate of each neutral mutation left to chance (genetic drift), the direction of evolutionary change is driven by which mutations occur, and so cannot be captured by models of change in the frequency of (existing) alleles alone.[13][15]

The origin-fixation view of population genetics generalizes this approach beyond strictly neutral mutations, and sees the rate at which a particular change happens as the product of the mutation rate and the fixation probability.[13]

Four processes

Selection

Natural selection, which includes sexual selection, is the fact that some traits make it more likely for an organism to survive and reproduce. Population genetics describes natural selection by defining fitness as a propensity or probability of survival and reproduction in a particular environment. The fitness is normally given by the symbol w=1-s where s is the selection coefficient. Natural selection acts on phenotypes, so population genetic models assume relatively simple relationships to predict the phenotype and hence fitness from the allele at one or a small number of loci. In this way, natural selection converts differences in the fitness of individuals with different phenotypes into changes in allele frequency in a population over successive generations.[citation needed]

Before the advent of population genetics, many biologists doubted that small differences in fitness were sufficient to make a large difference to evolution.[9] Population geneticists addressed this concern in part by comparing selection to genetic drift. Selection can overcome genetic drift when s is greater than 1 divided by the effective population size. When this criterion is met, the probability that a new advantageous mutant becomes fixed is approximately equal to 2s.[16][17] The time until fixation of such an allele depends little on genetic drift, and is approximately proportional to log(sN)/s.[18]

Dominance

Dominance means that the phenotypic and/or fitness effect of one allele at a locus depends on which allele is present in the second copy for that locus. Consider three genotypes at one locus, with the following fitness values[19]

Genotype: A1A1 A1A2 A2A2
Relative fitness: 1 1-hs 1-s
Population Genetics Glossary

s is the selection coefficient and h is the dominance coefficient. The value of h yields the following information:

h=0 A1 dominant, A2 recessive
h=1 A2 dominant, A1 recessive
0<h<1 incomplete dominance
h<0 overdominance
h>1 Underdominance

Epistasis

 
The logarithm of fitness as a function of the number of deleterious mutations. Synergistic epistasis is represented by the red line - each subsequent deleterious mutation has a larger proportionate effect on the organism's fitness. Antagonistic epistasis is in blue. The black line shows the non-epistatic case, where fitness is the product of the contributions from each of its loci.

Epistasis means that the phenotypic and/or fitness effect of an allele at one locus depends on which alleles are present at other loci. Selection does not act on a single locus, but on a phenotype that arises through development from a complete genotype.[20] However, many population genetics models of sexual species are "single locus" models, where the fitness of an individual is calculated as the product of the contributions from each of its loci—effectively assuming no epistasis.

In fact, the genotype to fitness landscape is more complex. Population genetics must either model this complexity in detail, or capture it by some simpler average rule. Empirically, beneficial mutations tend to have a smaller fitness benefit when added to a genetic background that already has high fitness: this is known as diminishing returns epistasis.[21] When deleterious mutations also have a smaller fitness effect on high fitness backgrounds, this is known as "synergistic epistasis". However, the effect of deleterious mutations tends on average to be very close to multiplicative, or can even show the opposite pattern, known as "antagonistic epistasis".[22]

Synergistic epistasis is central to some theories of the purging of mutation load[23] and to the evolution of sexual reproduction.

Mutation

Main article: Mutation
 
Drosophila melanogaster

Mutation is the ultimate source of genetic variation in the form of new alleles. In addition, mutation may influence the direction of evolution when there is mutation bias, i.e. different probabilities for different mutations to occur. For example, recurrent mutation that tends to be in the opposite direction to selection can lead to mutation–selection balance. At the molecular level, if mutation from G to A happens more often than mutation from A to G, then genotypes with A will tend to evolve.[24] Different insertion vs. deletion mutation biases in different taxa can lead to the evolution of different genome sizes.[25][26] Developmental or mutational biases have also been observed in morphological evolution.[27][28] For example, according to the phenotype-first theory of evolution, mutations can eventually cause the genetic assimilation of traits that were previously induced by the environment.[29][30]

Mutation bias effects are superimposed on other processes. If selection would favor either one out of two mutations, but there is no extra advantage to having both, then the mutation that occurs the most frequently is the one that is most likely to become fixed in a population.[31][32]

Mutation can have no effect, alter the product of a gene, or prevent the gene from functioning. Studies in the fly Drosophila melanogaster suggest that if a mutation changes a protein produced by a gene, this will probably be harmful, with about 70 percent of these mutations having damaging effects, and the remainder being either neutral or weakly beneficial.[33] Most loss of function mutations are selected against. But when selection is weak, mutation bias towards loss of function can affect evolution.[34] For example, pigments are no longer useful when animals live in the darkness of caves, and tend to be lost.[35] This kind of loss of function can occur because of mutation bias, and/or because the function had a cost, and once the benefit of the function disappeared, natural selection leads to the loss. Loss of sporulation ability in a bacterium during laboratory evolution appears to have been caused by mutation bias, rather than natural selection against the cost of maintaining sporulation ability.[36] When there is no selection for loss of function, the speed at which loss evolves depends more on the mutation rate than it does on the effective population size,[37] indicating that it is driven more by mutation bias than by genetic drift.

Mutations can involve large sections of DNA becoming duplicated, usually through genetic recombination.[38] This leads to copy-number variation within a population. Duplications are a major source of raw material for evolving new genes.[39] Other types of mutation occasionally create new genes from previously noncoding DNA.[40][41]

Genetic drift

Main article: Genetic drift

Genetic drift is a change in allele frequencies caused by random sampling.[42] That is, the alleles in the offspring are a random sample of those in the parents.[43] Genetic drift may cause gene variants to disappear completely, and thereby reduce genetic variability. In contrast to natural selection, which makes gene variants more common or less common depending on their reproductive success,[44] the changes due to genetic drift are not driven by environmental or adaptive pressures, and are equally likely to make an allele more common as less common.

The effect of genetic drift is larger for alleles present in few copies than when an allele is present in many copies. The population genetics of genetic drift are described using either branching processes or a diffusion equation describing changes in allele frequency.[45] These approaches are usually applied to the Wright-Fisher and Moran models of population genetics. Assuming genetic drift is the only evolutionary force acting on an allele, after t generations in many replicated populations, starting with allele frequencies of p and q, the variance in allele frequency across those populations is

 [46]

Ronald Fisher held the view that genetic drift plays at the most a minor role in evolution, and this remained the dominant view for several decades. No population genetics perspective have ever given genetic drift a central role by itself, but some have made genetic drift important in combination with another non-selective force. The shifting balance theory of Sewall Wright held that the combination of population structure and genetic drift was important. Motoo Kimura's neutral theory of molecular evolution claims that most genetic differences within and between populations are caused by the combination of neutral mutations and genetic drift.[47]

The role of genetic drift by means of sampling error in evolution has been criticized by John H Gillespie[48] and Will Provine,[49] who argue that selection on linked sites is a more important stochastic force, doing the work traditionally ascribed to genetic drift by means of sampling error. The mathematical properties of genetic draft are different from those of genetic drift.[50] The direction of the random change in allele frequency is autocorrelated across generations.[42]

Gene flow

 
Gene flow is the transfer of alleles from one population to another population through immigration of individuals. In this example, one of the birds from population A immigrates to population B, which has fewer of the dominant alleles, and through mating incorporates its alleles into the other population.
Main article: Gene flow

Because of physical barriers to migration, along with the limited tendency for individuals to move or spread (vagility), and tendency to remain or come back to natal place (philopatry), natural populations rarely all interbreed as may be assumed in theoretical random models (panmixy).[51] There is usually a geographic range within which individuals are more closely related to one another than those randomly selected from the general population. This is described as the extent to which a population is genetically structured.[52]

 
The Great Wall of China is an obstacle to gene flow of some terrestrial species.[53]

Genetic structuring can be caused by migration due to historical climate change, species range expansion or current availability of habitat. Gene flow is hindered by mountain ranges, oceans and deserts or even man-made structures such as the Great Wall of China, which has hindered the flow of plant genes.[53]

Gene flow is the exchange of genes between populations or species, breaking down the structure. Examples of gene flow within a species include the migration and then breeding of organisms, or the exchange of pollen. Gene transfer between species includes the formation of hybrid organisms and horizontal gene transfer. Population genetic models can be used to identify which populations show significant genetic isolation from one another, and to reconstruct their history.[54]

Subjecting a population to isolation leads to inbreeding depression. Migration into a population can introduce new genetic variants,[55] potentially contributing to evolutionary rescue. If a significant proportion of individuals or gametes migrate, it can also change allele frequencies, e.g. giving rise to migration load.[56]

In the presence of gene flow, other barriers to hybridization between two diverging populations of an outcrossing species are required for the populations to become new species.

Horizontal gene transfer

 
Current tree of life showing vertical and horizontal gene transfers.
Main article: Horizontal gene transfer

Horizontal gene transfer is the transfer of genetic material from one organism to another organism that is not its offspring; this is most common among prokaryotes.[57] In medicine, this contributes to the spread of antibiotic resistance, as when one bacteria acquires resistance genes it can rapidly transfer them to other species.[58] Horizontal transfer of genes from bacteria to eukaryotes such as the yeast Saccharomyces cerevisiae and the adzuki bean beetle Callosobruchus chinensis may also have occurred.[59][60] An example of larger-scale transfers are the eukaryotic bdelloid rotifers, which appear to have received a range of genes from bacteria, fungi, and plants.[61] Viruses can also carry DNA between organisms, allowing transfer of genes even across biological domains.[62] Large-scale gene transfer has also occurred between the ancestors of eukaryotic cells and prokaryotes, during the acquisition of chloroplasts and mitochondria.[63]

Linkage

If all genes are in linkage equilibrium, the effect of an allele at one locus can be averaged across the gene pool at other loci. In reality, one allele is frequently found in linkage disequilibrium with genes at other loci, especially with genes located nearby on the same chromosome. Recombination breaks up this linkage disequilibrium too slowly to avoid genetic hitchhiking, where an allele at one locus rises to high frequency because it is linked to an allele under selection at a nearby locus. Linkage also slows down the rate of adaptation, even in sexual populations.[64][65][66] The effect of linkage disequilibrium in slowing down the rate of adaptive evolution arises from a combination of the Hill–Robertson effect (delays in bringing beneficial mutations together) and background selection (delays in separating beneficial mutations from deleterious hitchhikers).

Linkage is a problem for population genetic models that treat one gene locus at a time. It can, however, be exploited as a method for detecting the action of natural selection via selective sweeps.

In the extreme case of an asexual population, linkage is complete, and population genetic equations can be derived and solved in terms of a travelling wave of genotype frequencies along a simple fitness landscape.[67] Most microbes, such as bacteria, are asexual. The population genetics of their adaptation have two contrasting regimes. When the product of the beneficial mutation rate and population size is small, asexual populations follow a "successional regime" of origin-fixation dynamics, with adaptation rate strongly dependent on this product. When the product is much larger, asexual populations follow a "concurrent mutations" regime with adaptation rate less dependent on the product, characterized by clonal interference and the appearance of a new beneficial mutation before the last one has fixed.

Applications

Explaining levels of genetic variation

Neutral theory predicts that the level of nucleotide diversity in a population will be proportional to the product of the population size and the neutral mutation rate. The fact that levels of genetic diversity vary much less than population sizes do is known as the "paradox of variation".[68] While high levels of genetic diversity were one of the original arguments in favor of neutral theory, the paradox of variation has been one of the strongest arguments against neutral theory.

It is clear that levels of genetic diversity vary greatly within a species as a function of local recombination rate, due to both genetic hitchhiking and background selection. Most current solutions to the paradox of variation invoke some level of selection at linked sites.[69] For example, one analysis suggests that larger populations have more selective sweeps, which remove more neutral genetic diversity.[70] A negative correlation between mutation rate and population size may also contribute.[71]

Life history affects genetic diversity more than population history does, e.g. r-strategists have more genetic diversity.[69]

Detecting selection

Population genetics models are used to infer which genes are undergoing selection. One common approach is to look for regions of high linkage disequilibrium and low genetic variance along the chromosome, to detect recent selective sweeps.

A second common approach is the McDonald–Kreitman test which compares the amount of variation within a species (polymorphism) to the divergence between species (substitutions) at two types of sites; one assumed to be neutral. Typically, synonymous sites are assumed to be neutral.[72] Genes undergoing positive selection have an excess of divergent sites relative to polymorphic sites. The test can also be used to obtain a genome-wide estimate of the proportion of substitutions that are fixed by positive selection, α.[73][74] According to the neutral theory of molecular evolution, this number should be near zero. High numbers have therefore been interpreted as a genome-wide falsification of neutral theory.[75]

Demographic inference

The simplest test for population structure in a sexually reproducing, diploid species, is to see whether genotype frequencies follow Hardy-Weinberg proportions as a function of allele frequencies. For example, in the simplest case of a single locus with two alleles denoted A and a at frequencies p and q, random mating predicts freq(AA) = p2 for the AA homozygotes, freq(aa) = q2 for the aa homozygotes, and freq(Aa) = 2pq for the heterozygotes. In the absence of population structure, Hardy-Weinberg proportions are reached within 1-2 generations of random mating. More typically, there is an excess of homozygotes, indicative of population structure. The extent of this excess can be quantified as the inbreeding coefficient, F.

Individuals can be clustered into K subpopulations.[76][77] The degree of population structure can then be calculated using FST, which is a measure of the proportion of genetic variance that can be explained by population structure. Genetic population structure can then be related to geographic structure, and genetic admixture can be detected.

Coalescent theory relates genetic diversity in a sample to demographic history of the population from which it was taken. It normally assumes neutrality, and so sequences from more neutrally-evolving portions of genomes are therefore selected for such analyses. It can be used to infer the relationships between species (phylogenetics), as well as the population structure, demographic history (e.g. population bottlenecks, population growth), biological dispersal, source–sink dynamics[78] and introgression within a species.

Another approach to demographic inference relies on the allele frequency spectrum.[79]

Evolution of genetic systems

By assuming that there are loci that control the genetic system itself, population genetic models are created to describe the evolution of dominance and other forms of robustness, the evolution of sexual reproduction and recombination rates, the evolution of mutation rates, the evolution of evolutionary capacitors, the evolution of costly signalling traits, the evolution of ageing, and the evolution of co-operation. For example, most mutations are deleterious, so the optimal mutation rate for a species may be a trade-off between the damage from a high deleterious mutation rate and the metabolic costs of maintaining systems to reduce the mutation rate, such as DNA repair enzymes.[80]

One important aspect of such models is that selection is only strong enough to purge deleterious mutations and hence overpower mutational bias towards degradation if the selection coefficient s is greater than the inverse of the effective population size. This is known as the drift barrier and is related to the nearly neutral theory of molecular evolution. Drift barrier theory predicts that species with large effective population sizes will have highly streamlined, efficient genetic systems, while those with small population sizes will have bloated and complex genomes containing for example introns and transposable elements.[81] However, somewhat paradoxically, species with large population sizes might be so tolerant to the consequences of certain types of errors that they evolve higher error rates, e.g. in transcription and translation, than small populations.[82]

See also

References

  1. ^ "Population genetics - Latest research and news". www.nature.com. Retrieved 2018-01-29.
  2. ^ Servedio, Maria R.; Brandvain, Yaniv; Dhole, Sumit; Fitzpatrick, Courtney L.; Goldberg, Emma E.; Stern, Caitlin A.; Van Cleve, Jeremy; Yeh, D. Justin (9 December 2014). "Not Just a Theory—The Utility of Mathematical Models in Evolutionary Biology". PLOS Biology. 12 (12): e1002017. doi:10.1371/journal.pbio.1002017. PMC 4260780. PMID 25489940.
  3. ^ Ewens, W.J. (2004). Mathematical Population Genetics (2nd ed.). New York: Springer. ISBN 978-0-387-20191-7.
  4. ^ a b c Bowler, Peter J. (2003). Evolution : the history of an idea (3rd ed.). Berkeley: University of California Press. pp. 325–339. ISBN 978-0-520-23693-6.
  5. ^ a b c Larson, Edward J. (2004). Evolution : the remarkable history of a scientific theory (Modern Library ed.). New York: Modern Library. pp. 221–243. ISBN 978-0-679-64288-6.
  6. ^ Beatty, John (1986). "The Synthesis and the Synthetic Theory". Integrating Scientific Disciplines. Science and Philosophy. Vol. 2. Springer Netherlands. pp. 125–135. doi:10.1007/978-94-010-9435-1_7. ISBN 9789024733422.
  7. ^ Mayr, Ernst; Provine, William B., eds. (1998). The Evolutionary synthesis : perspectives on the unification of biology ([New ed]. ed.). Cambridge, Massachusetts: Harvard University Press. pp. 295–298. ISBN 9780674272262.
  8. ^ a b Provine, W. B. (1988). "Progress in evolution and meaning in life". Evolutionary progress. University of Chicago Press. pp. 49–79.
  9. ^ a b Provine, William B. (1978). "The role of mathematical population geneticists in the evolutionary synthesis of the 1930s and 1940s". Studies of the History of Biology. 2: 167–192. PMID 11610409.
  10. ^ Ford, E. B. (1975) [1964]. Ecological genetics (4th ed.). London: Chapman and Hall. pp. 1ff.
  11. ^ Mayr, Ernst (1988). Toward a New Philosophy of Biology: Observations of an Evolutionist. Cambridge, Massachusetts: Belknap Press of Harvard University Press. p. 402. ISBN 978-0-674-89665-9.
  12. ^ Mayr, Ernst; Provine, William B., eds. (1998). The Evolutionary Synthesis : perspectives on the unification of biology ([New ed]. ed.). Cambridge, Massachusetts: Harvard University Press. pp. 338–341. ISBN 9780674272262.
  13. ^ a b c McCandlish, David M.; Stoltzfus, Arlin (September 2014). "Modeling Evolution Using the Probability of Fixation: History and Implications". The Quarterly Review of Biology. 89 (3): 225–252. doi:10.1086/677571. PMID 25195318. S2CID 19619966.
  14. ^ Crow, James F. (2010). "Wright and Fisher on Inbreeding and Random Drift". Genetics. 184 (3): 609–611. doi:10.1534/genetics.109.110023. ISSN 0016-6731. PMC 2845331. PMID 20332416.
  15. ^ Casillas, Sònia; Barbadilla, Antonio (2017). "Molecular Population Genetics". Genetics. 205 (3): 1003–1035. doi:10.1534/genetics.116.196493. PMC 5340319. PMID 28270526.
  16. ^ Haldane, J. B. S. (1927). "A Mathematical Theory of Natural and Artificial Selection, Part V: Selection and Mutation". Mathematical Proceedings of the Cambridge Philosophical Society. 23 (7): 838–844. Bibcode:1927PCPS...23..838H. doi:10.1017/S0305004100015644. S2CID 86716613.
  17. ^ Orr, H. A. (2010). "The population genetics of beneficial mutations". Philosophical Transactions of the Royal Society B: Biological Sciences. 365 (1544): 1195–1201. doi:10.1098/rstb.2009.0282. PMC 2871816. PMID 20308094.
  18. ^ Hermisson, J.; Pennings, P. S. (2005). "Soft sweeps: molecular population genetics of adaptation from standing genetic variation". Genetics. 169 (4): 2335–2352. doi:10.1534/genetics.104.036947. PMC 1449620. PMID 15716498.
  19. ^ Gillespie, John (2004). Population Genetics: A Concise Guide (2nd ed.). Johns Hopkins University Press. ISBN 978-0-8018-8008-7.
  20. ^ Miko, I. (2008). "Epistasis: Gene interaction and phenotype effects". Nature Education. 1 (1): 197.
  21. ^ Berger, D.; Postma, E. (13 October 2014). "Biased Estimates of Diminishing-Returns Epistasis? Empirical Evidence Revisited". Genetics. 198 (4): 1417–1420. doi:10.1534/genetics.114.169870. PMC 4256761. PMID 25313131.
  22. ^ Kouyos, Roger D.; Silander, Olin K.; Bonhoeffer, Sebastian (June 2007). "Epistasis between deleterious mutations and the evolution of recombination". Trends in Ecology & Evolution. 22 (6): 308–315. doi:10.1016/j.tree.2007.02.014. PMID 17337087.
  23. ^ Crow, J. F. (5 August 1997). "The high spontaneous mutation rate: is it a health risk?". Proceedings of the National Academy of Sciences of the United States of America. 94 (16): 8380–8386. Bibcode:1997PNAS...94.8380C. doi:10.1073/pnas.94.16.8380. PMC 33757. PMID 9237985.
  24. ^ Smith, N. G. C.; Webster, M. T.; Ellegren, H. (2002). "Deterministic Mutation Rate Variation in the Human Genome". Genome Research. 12 (9): 1350–1356. doi:10.1101/gr.220502. PMC 186654. PMID 12213772.
  25. ^ Petrov, D. A. (2000). "Evidence for DNA Loss as a Determinant of Genome Size". Science. 287 (5455): 1060–1062. Bibcode:2000Sci...287.1060P. doi:10.1126/science.287.5455.1060. ISSN 0036-8075. PMID 10669421.
  26. ^ Petrov, D. A. (2002). "DNA loss and evolution of genome size in Drosophila". Genetica. 115 (1): 81–91. doi:10.1023/A:1016076215168. PMID 12188050. S2CID 5314242.
  27. ^ Kiontke, K.; Barrière, A.; Kolotuev, I.; Podbilewicz, B.; Sommer, R.; Fitch, D. H. A.; Félix, M. A. (2007). "Trends, stasis, and drift in the evolution of nematode vulva development". Current Biology. 17 (22): 1925–1937. doi:10.1016/j.cub.2007.10.061. PMID 18024125. S2CID 4503181.
  28. ^ Braendle, C.; Baer, C. F.; Félix, M. A. (2010). Barsh, Gregory S. (ed.). "Bias and Evolution of the Mutationally Accessible Phenotypic Space in a Developmental System". PLOS Genetics. 6 (3): e1000877. doi:10.1371/journal.pgen.1000877. PMC 2837400. PMID 20300655.
  29. ^ Palmer, RA (2004). "Symmetry breaking and the evolution of development". Science. 306 (5697): 828–833. Bibcode:2004Sci...306..828P. CiteSeerX 10.1.1.631.4256. doi:10.1126/science.1103707. PMID 15514148. S2CID 32054147.
  30. ^ West-Eberhard, M-J. (2003). Developmental plasticity and evolution. New York: Oxford University Press. ISBN 978-0-19-512235-0.
  31. ^ Stoltzfus, A.; Yampolsky, L. Y. (2009). "Climbing Mount Probable: Mutation as a Cause of Nonrandomness in Evolution". Journal of Heredity. 100 (5): 637–647. doi:10.1093/jhered/esp048. PMID 19625453.
  32. ^ Yampolsky, L. Y.; Stoltzfus, A. (2001). "Bias in the introduction of variation as an orienting factor in evolution". Evol Dev. 3 (2): 73–83. doi:10.1046/j.1525-142x.2001.003002073.x. PMID 11341676. S2CID 26956345.
  33. ^ Sawyer, S. A.; Parsch, J.; Zhang, Z.; Hartl, D. L. (2007). "Prevalence of positive selection among nearly neutral amino acid replacements in Drosophila". Proceedings of the National Academy of Sciences. 104 (16): 6504–6510. doi:10.1073/pnas.0701572104. ISSN 0027-8424. PMC 1871816. PMID 17409186.
  34. ^ Haldane, J. B. S. (1933). "The Part Played by Recurrent Mutation in Evolution". American Naturalist. 67 (708): 5–19. doi:10.1086/280465. JSTOR 2457127. S2CID 84059440.
  35. ^ Protas, Meredith; Conrad, M.; Gross, J. B.; Tabin, C.; Borowsky, R (2007). "Regressive evolution in the Mexican cave tetra, Astyanax mexicanus". Current Biology. 17 (5): 452–454. doi:10.1016/j.cub.2007.01.051. PMC 2570642. PMID 17306543.
  36. ^ Maughan, H.; Masel, J.; Birky, W. C.; Nicholson, W. L. (2007). "The roles of mutation accumulation and selection in loss of sporulation in experimental populations of Bacillus subtilis". Genetics. 177 (2): 937–948. doi:10.1534/genetics.107.075663. PMC 2034656. PMID 17720926.
  37. ^ Masel, J.; King, O. D.; Maughan, H. (2007). "The loss of adaptive plasticity during long periods of environmental stasis". American Naturalist. 169 (1): 38–46. doi:10.1086/510212. PMC 1766558. PMID 17206583.
  38. ^ Hastings, P. J.; Lupski, J. R.; Rosenberg, S. M.; Ira, G. (2009). "Mechanisms of change in gene copy number". Nature Reviews Genetics. 10 (8): 551–564. doi:10.1038/nrg2593. PMC 2864001. PMID 19597530.
  39. ^ M., Long; Betrán, E.; Thornton, K.; Wang, W. (November 2003). "The origin of new genes: glimpses from the young and old". Nat. Rev. Genet. 4 (11): 865–75. doi:10.1038/nrg1204. PMID 14634634. S2CID 33999892.
  40. ^ Liu, N.; Okamura, K.; Tyler, D. M.; Phillips; Chung; Lai (2008). "The evolution and functional diversification of animal microRNA genes". Cell Research. 18 (10): 985–996. doi:10.1038/cr.2008.278. PMC 2712117. PMID 18711447.
  41. ^ McLysaght, Aoife; Hurst, Laurence D. (25 July 2016). "Open questions in the study of de novo genes: what, how and why". Nature Reviews Genetics. 17 (9): 567–578. doi:10.1038/nrg.2016.78. PMID 27452112. S2CID 6033249.
  42. ^ a b Masel, J. (2011). "Genetic drift". Current Biology. 21 (20): R837–R838. doi:10.1016/j.cub.2011.08.007. PMID 22032182.
  43. ^ Futuyma, Douglas (1998). Evolutionary Biology. Sinauer Associates. p. Glossary. ISBN 978-0-87893-189-7.
  44. ^ Avers, Charlotte (1989). Process and Pattern in Evolution. Oxford University Press.
  45. ^ Wahl, L. M. (2011). "Fixation when N and s Vary: Classic Approaches Give Elegant New Results". Genetics. 188 (4): 783–785. doi:10.1534/genetics.111.131748. PMC 3176088. PMID 21828279.
  46. ^ Barton, Nicholas H.; Briggs, Derek E. G.; Eisen, Jonathan A.; Goldstein, David B.; Patel, Nipam H. (2007). Evolution. Cold Spring Harbor Laboratory Press. p. 417. ISBN 978-0-87969-684-9.
  47. ^ Futuyma, Douglas (1998). Evolutionary Biology. Sinauer Associates. p. 320. ISBN 978-0-87893-189-7.
  48. ^ Gillespie, J. H. (2000). "Genetic Drift in an Infinite Population: The Pseudohitchhiking Model". Genetics. 155 (2): 909–919. doi:10.1093/genetics/155.2.909. PMC 1461093. PMID 10835409.
  49. ^ Provine, William B. The "Random Genetic Drift" Fallacy. CreateSpace.
  50. ^ Neher, Richard A.; Shraiman, Boris I. (August 2011). "Genetic Draft and Quasi-Neutrality in Large Facultatively Sexual Populations". Genetics. 188 (4): 975–996. arXiv:1108.1635. doi:10.1534/genetics.111.128876. ISSN 0016-6731. PMC 3176096. PMID 21625002.
  51. ^ Buston, P. M.; Pilkington, J. G.; et al. (2007). "Are clownfish groups composed of close relatives? An analysis of microsatellite DNA vraiation in Amphiprion percula". Molecular Ecology. 12 (3): 733–742. doi:10.1046/j.1365-294X.2003.01762.x. PMID 12675828. S2CID 35546810.
  52. ^ Repaci, V.; Stow, A. J.; Briscoe, D. A. (2007). "Fine-scale genetic structure, co-founding and multiple mating in the Australian allodapine bee (Ramphocinclus brachyurus)". Journal of Zoology. 270 (4): 687–691. doi:10.1111/j.1469-7998.2006.00191.x.
  53. ^ a b Su, H.; Qu, L.-J.; He, K.; Zhang, Z.; Wang, J; Chen, Z.; Gu, H. (2003). "The Great Wall of China: a physical barrier to gene flow?". Heredity. 90 (3): 212–219. doi:10.1038/sj.hdy.6800237. ISSN 0018-067X. PMID 12634804. S2CID 13367320.
  54. ^ Gravel, S. (2012). "Population Genetics Models of Local Ancestry". Genetics. 1202 (2): 607–619. arXiv:1202.4811. Bibcode:2012arXiv1202.4811G. doi:10.1534/genetics.112.139808. PMC 3374321. PMID 22491189.
  55. ^ Morjan, C.; Rieseberg, L. (2004). "How species evolve collectively: implications of gene flow and selection for the spread of advantageous alleles". Molecular Ecology. 13 (6): 1341–56. doi:10.1111/j.1365-294X.2004.02164.x. PMC 2600545. PMID 15140081.
  56. ^ Bolnick, Daniel I.; Nosil, Patrik (September 2007). "Natural Selection in Populations Subject to a Migration Load". Evolution. 61 (9): 2229–2243. doi:10.1111/j.1558-5646.2007.00179.x. PMID 17767592. S2CID 25685919.
  57. ^ Boucher, Yan; Douady, Christophe J.; Papke, R. Thane; Walsh, David A.; Boudreau, Mary Ellen R.; Nesbø, Camilla L.; Case, Rebecca J.; Doolittle, W. Ford (2003). "Lateral Gene Transfer and the Origins of Prokaryotic Groups". Annual Review of Genetics. 37 (1): 283–328. doi:10.1146/annurev.genet.37.050503.084247. ISSN 0066-4197. PMID 14616063.
  58. ^ Walsh, T. (2006). "Combinatorial genetic evolution of multiresistance". Current Opinion in Microbiology. 9 (5): 476–82. doi:10.1016/j.mib.2006.08.009. PMID 16942901.
  59. ^ Kondo, N.; Nikoh, N.; Ijichi, N.; Shimada, M.; Fukatsu, T. (2002). "Genome fragment of Wolbachia endosymbiont transferred to X chromosome of host insect". Proceedings of the National Academy of Sciences. 99 (22): 14280–14285. Bibcode:2002PNAS...9914280K. doi:10.1073/pnas.222228199. ISSN 0027-8424. PMC 137875. PMID 12386340.
  60. ^ Sprague, G. (1991). "Genetic exchange between kingdoms". Current Opinion in Genetics & Development. 1 (4): 530–533. doi:10.1016/S0959-437X(05)80203-5. PMID 1822285.
  61. ^ Gladyshev, E. A.; Meselson, M.; Arkhipova, I. R. (2008). "Massive Horizontal Gene Transfer in Bdelloid Rotifers". Science. 320 (5880): 1210–1213. Bibcode:2008Sci...320.1210G. doi:10.1126/science.1156407. ISSN 0036-8075. PMID 18511688. S2CID 11862013.
  62. ^ Baldo, A.; McClure, M. (1 September 1999). "Evolution and horizontal transfer of dUTPase-encoding genes in viruses and their hosts". Journal of Virology. 73 (9): 7710–7721. doi:10.1128/JVI.73.9.7710-7721.1999. PMC 104298. PMID 10438861.
  63. ^ Poole, A.; Penny, D. (2007). "Evaluating hypotheses for the origin of eukaryotes". BioEssays. 29 (1): 74–84. doi:10.1002/bies.20516. PMID 17187354.
  64. ^ Weissman, D. B.; Hallatschek, O. (15 January 2014). "The Rate of Adaptation in Large Sexual Populations with Linear Chromosomes". Genetics. 196 (4): 1167–1183. doi:10.1534/genetics.113.160705. PMC 3982688. PMID 24429280.
  65. ^ Weissman, Daniel B.; Barton, Nicholas H.; McVean, Gil (7 June 2012). "Limits to the Rate of Adaptive Substitution in Sexual Populations". PLOS Genetics. 8 (6): e1002740. doi:10.1371/journal.pgen.1002740. PMC 3369949. PMID 22685419.
  66. ^ Neher, R. A.; Shraiman, B. I.; Fisher, D. S. (30 November 2009). "Rate of Adaptation in Large Sexual Populations". Genetics. 184 (2): 467–481. arXiv:1108.3464. doi:10.1534/genetics.109.109009. PMC 2828726. PMID 19948891.
  67. ^ Desai, Michael M.; Fisher, Daniel S. (2007). "Beneficial Mutation Selection Balance and the Effect of Linkage on Positive Selection". Genetics. 176 (3): 1759–1798. doi:10.1534/genetics.106.067678. PMC 1931526. PMID 17483432.
  68. ^ Lewontin, R. C. (1973). The genetic basis of evolutionary change ([4th printing.] ed.). New York: Columbia University Press. ISBN 978-0231033923.
  69. ^ a b Ellegren, Hans; Galtier, Nicolas (6 June 2016). "Determinants of genetic diversity". Nature Reviews Genetics. 17 (7): 422–433. doi:10.1038/nrg.2016.58. PMID 27265362. S2CID 23531428.
  70. ^ Corbett-Detig, Russell B.; Hartl, Daniel L.; Sackton, Timothy B.; Barton, Nick H. (10 April 2015). "Natural Selection Constrains Neutral Diversity across A Wide Range of Species". PLOS Biology. 13 (4): e1002112. doi:10.1371/journal.pbio.1002112. PMC 4393120. PMID 25859758.
  71. ^ Sung, W.; Ackerman, M. S.; Miller, S. F.; Doak, T. G.; Lynch, M. (17 October 2012). "Drift-barrier hypothesis and mutation-rate evolution" (PDF). Proceedings of the National Academy of Sciences. 109 (45): 18488–18492. Bibcode:2012PNAS..10918488S. doi:10.1073/pnas.1216223109. PMC 3494944. PMID 23077252.
  72. ^ Charlesworth, J. Eyre-Walker (2008). "The McDonald–Kreitman Test and Slightly Deleterious Mutations". Molecular Biology and Evolution. 25 (6): 1007–1015. doi:10.1093/molbev/msn005. PMID 18195052.
  73. ^ Eyre-Walker, A. (2006). "The genomic rate of adaptive evolution" (PDF). Trends in Ecology and Evolution. 21 (10): 569–575. doi:10.1016/j.tree.2006.06.015. PMID 16820244.
  74. ^ Smith, N. G. C.; Eyre-Walker, A. (2002). "Adaptive protein evolution in Drosophila". Nature. 415 (6875): 1022–1024. Bibcode:2002Natur.415.1022S. doi:10.1038/4151022a. PMID 11875568. S2CID 4426258.
  75. ^ Hahn, M. W. (2008). "Toward a selection theory of molecular evolution". Evolution. 62 (2): 255–265. doi:10.1111/j.1558-5646.2007.00308.x. PMID 18302709. S2CID 5986211.
  76. ^ Pritchard, J. K.; Stephens, M.; Donnelly, P. (June 2000). "Inference of population structure using multilocus genotype data". Genetics. 155 (2): 945–959. doi:10.1093/genetics/155.2.945. ISSN 0016-6731. PMC 1461096. PMID 10835412.
  77. ^ Verity, Robert; Nichols, Richard A. (August 2016). "Estimating the Number of Subpopulations (K) in Structured Populations". Genetics. 203 (4): 1827–1839. doi:10.1534/genetics.115.180992. ISSN 0016-6731. PMC 4981280. PMID 27317680.
  78. ^ Manlik, Oliver; Chabanne, Delphine; Daniel, Claire; Bejder, Lars; Allen, Simon J.; Sherwin, William B. (13 November 2018). "Demography and genetics suggest reversal of dolphin source–sink dynamics, with implications for conservation". Marine Mammal Science. 35 (3): 732–759. doi:10.1111/mms.12555. S2CID 92108810.
  79. ^ Gutenkunst, Ryan N.; Hernandez, Ryan D.; Williamson, Scott H.; Bustamante, Carlos D.; McVean, Gil (23 October 2009). "Inferring the Joint Demographic History of Multiple Populations from Multidimensional SNP Frequency Data". PLOS Genetics. 5 (10): e1000695. arXiv:0909.0925. doi:10.1371/journal.pgen.1000695. PMC 2760211. PMID 19851460.
  80. ^ Sniegowski, P. (2000). Gerrish P.; Johnson T;. Shaver A. "The evolution of mutation rates: separating causes from consequences". BioEssays. 22 (12): 1057–1066. doi:10.1002/1521-1878(200012)22:12<1057::AID-BIES3>3.0.CO;2-W. PMID 11084621. S2CID 36771934.
  81. ^ Lynch, Michael; Conery, John S. (2003). "The origins of genome complexity". Science. 302 (5649): 1401–1404. Bibcode:2003Sci...302.1401L. CiteSeerX 10.1.1.135.974. doi:10.1126/science.1089370. PMID 14631042. S2CID 11246091.
  82. ^ Rajon, E.; Masel, J. (3 January 2011). "Evolution of molecular error rates and the consequences for evolvability". Proceedings of the National Academy of Sciences. 108 (3): 1082–1087. Bibcode:2011PNAS..108.1082R. doi:10.1073/pnas.1012918108. PMC 3024668. PMID 21199946.

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January 10, 2023
population, genetics, subfield, genetics, that, deals, with, genetic, differences, within, between, populations, part, evolutionary, biology, studies, this, branch, biology, examine, such, phenomena, adaptation, speciation, population, structure, vital, ingred. Population genetics is a subfield of genetics that deals with genetic differences within and between populations and is a part of evolutionary biology Studies in this branch of biology examine such phenomena as adaptation speciation and population structure 1 Population genetics was a vital ingredient in the emergence of the modern evolutionary synthesis Its primary founders were Sewall Wright J B S Haldane and Ronald Fisher who also laid the foundations for the related discipline of quantitative genetics Traditionally a highly mathematical discipline modern population genetics encompasses theoretical laboratory and field work Population genetic models are used both for statistical inference from DNA sequence data and for proof disproof of concept 2 What sets population genetics apart from newer more phenotypic approaches to modelling evolution such as evolutionary game theory and adaptive dynamics is its emphasis on such genetic phenomena as dominance epistasis the degree to which genetic recombination breaks linkage disequilibrium and the random phenomena of mutation and genetic drift This makes it appropriate for comparison to population genomics data Contents 1 History 1 1 Modern synthesis 1 2 Neutral theory and origin fixation dynamics 2 Four processes 2 1 Selection 2 1 1 Dominance 2 1 2 Epistasis 2 2 Mutation 2 3 Genetic drift 2 4 Gene flow 2 4 1 Horizontal gene transfer 3 Linkage 4 Applications 4 1 Explaining levels of genetic variation 4 2 Detecting selection 4 3 Demographic inference 4 4 Evolution of genetic systems 5 See also 6 References 7 External linksHistory EditPopulation genetics began as a reconciliation of Mendelian inheritance and biostatistics models Natural selection will only cause evolution if there is enough genetic variation in a population Before the discovery of Mendelian genetics one common hypothesis was blending inheritance But with blending inheritance genetic variance would be rapidly lost making evolution by natural or sexual selection implausible The Hardy Weinberg principle provides the solution to how variation is maintained in a population with Mendelian inheritance According to this principle the frequencies of alleles variations in a gene will remain constant in the absence of selection mutation migration and genetic drift 3 The typical white bodied form of the peppered moth Industrial melanism the black bodied form of the peppered moth appeared in polluted areas The next key step was the work of the British biologist and statistician Ronald Fisher In a series of papers starting in 1918 and culminating in his 1930 book The Genetical Theory of Natural Selection Fisher showed that the continuous variation measured by the biometricians could be produced by the combined action of many discrete genes and that natural selection could change allele frequencies in a population resulting in evolution In a series of papers beginning in 1924 another British geneticist J B S Haldane worked out the mathematics of allele frequency change at a single gene locus under a broad range of conditions Haldane also applied statistical analysis to real world examples of natural selection such as peppered moth evolution and industrial melanism and showed that selection coefficients could be larger than Fisher assumed leading to more rapid adaptive evolution as a camouflage strategy following increased pollution 4 5 The American biologist Sewall Wright who had a background in animal breeding experiments focused on combinations of interacting genes and the effects of inbreeding on small relatively isolated populations that exhibited genetic drift In 1932 Wright introduced the concept of an adaptive landscape and argued that genetic drift and inbreeding could drive a small isolated sub population away from an adaptive peak allowing natural selection to drive it towards different adaptive peaks citation needed The work of Fisher Haldane and Wright founded the discipline of population genetics This integrated natural selection with Mendelian genetics which was the critical first step in developing a unified theory of how evolution worked 4 5 John Maynard Smith was Haldane s pupil whilst W D Hamilton was influenced by the writings of Fisher The American George R Price worked with both Hamilton and Maynard Smith American Richard Lewontin and Japanese Motoo Kimura were influenced by Wright and Haldane citation needed Modern synthesis Edit Main article Modern synthesis 20th century The mathematics of population genetics were originally developed as the beginning of the modern synthesis Authors such as Beatty 6 have asserted that population genetics defines the core of the modern synthesis For the first few decades of the 20th century most field naturalists continued to believe that Lamarckism and orthogenesis provided the best explanation for the complexity they observed in the living world 7 During the modern synthesis these ideas were purged and only evolutionary causes that could be expressed in the mathematical framework of population genetics were retained 8 Consensus was reached as to which evolutionary factors might influence evolution but not as to the relative importance of the various factors 8 Theodosius Dobzhansky a postdoctoral worker in T H Morgan s lab had been influenced by the work on genetic diversity by Russian geneticists such as Sergei Chetverikov He helped to bridge the divide between the foundations of microevolution developed by the population geneticists and the patterns of macroevolution observed by field biologists with his 1937 book Genetics and the Origin of Species Dobzhansky examined the genetic diversity of wild populations and showed that contrary to the assumptions of the population geneticists these populations had large amounts of genetic diversity with marked differences between sub populations The book also took the highly mathematical work of the population geneticists and put it into a more accessible form Many more biologists were influenced by population genetics via Dobzhansky than were able to read the highly mathematical works in the original 9 In Great Britain E B Ford the pioneer of ecological genetics 10 continued throughout the 1930s and 1940s to empirically demonstrate the power of selection due to ecological factors including the ability to maintain genetic diversity through genetic polymorphisms such as human blood types Ford s work in collaboration with Fisher contributed to a shift in emphasis during the modern synthesis towards natural selection as the dominant force 4 5 11 12 Neutral theory and origin fixation dynamics Edit The original modern synthesis view of population genetics assumes that mutations provide ample raw material and focuses only on the change in frequency of alleles within populations 13 The main processes influencing allele frequencies are natural selection genetic drift gene flow and recurrent mutation Fisher and Wright had some fundamental disagreements about the relative roles of selection and drift 14 The availability of molecular data on all genetic differences led to the neutral theory of molecular evolution In this view many mutations are deleterious and so never observed and most of the remainder are neutral i e are not under selection With the fate of each neutral mutation left to chance genetic drift the direction of evolutionary change is driven by which mutations occur and so cannot be captured by models of change in the frequency of existing alleles alone 13 15 The origin fixation view of population genetics generalizes this approach beyond strictly neutral mutations and sees the rate at which a particular change happens as the product of the mutation rate and the fixation probability 13 Four processes EditSelection Edit Natural selection which includes sexual selection is the fact that some traits make it more likely for an organism to survive and reproduce Population genetics describes natural selection by defining fitness as a propensity or probability of survival and reproduction in a particular environment The fitness is normally given by the symbol w 1 s where s is the selection coefficient Natural selection acts on phenotypes so population genetic models assume relatively simple relationships to predict the phenotype and hence fitness from the allele at one or a small number of loci In this way natural selection converts differences in the fitness of individuals with different phenotypes into changes in allele frequency in a population over successive generations citation needed Before the advent of population genetics many biologists doubted that small differences in fitness were sufficient to make a large difference to evolution 9 Population geneticists addressed this concern in part by comparing selection to genetic drift Selection can overcome genetic drift when s is greater than 1 divided by the effective population size When this criterion is met the probability that a new advantageous mutant becomes fixed is approximately equal to 2s 16 17 The time until fixation of such an allele depends little on genetic drift and is approximately proportional to log sN s 18 Dominance Edit Dominance means that the phenotypic and or fitness effect of one allele at a locus depends on which allele is present in the second copy for that locus Consider three genotypes at one locus with the following fitness values 19 Genotype A1A1 A1A2 A2A2Relative fitness 1 1 hs 1 sPopulation Genetics Glossaryspecies a group of closely related organisms that are capable of interbreeding and producing fertile offspring population the total number of individuals of a particular species in a given area interbreed the ability to breed with another species homo sapiens with homo neanderthal gene pool the collective genetic information contained within a population of sexually reproducing organisms allele frequency the frequency or proportion of a particular allele of a gene within a population hardy weinberg principle an equation linking allele frequency to genotype frequency in a population p2 2pq q2 1s is the selection coefficient and h is the dominance coefficient The value of h yields the following information h 0 A1 dominant A2 recessiveh 1 A2 dominant A1 recessive0 lt h lt 1 incomplete dominanceh lt 0 overdominanceh gt 1 UnderdominanceEpistasis Edit The logarithm of fitness as a function of the number of deleterious mutations Synergistic epistasis is represented by the red line each subsequent deleterious mutation has a larger proportionate effect on the organism s fitness Antagonistic epistasis is in blue The black line shows the non epistatic case where fitness is the product of the contributions from each of its loci Epistasis means that the phenotypic and or fitness effect of an allele at one locus depends on which alleles are present at other loci Selection does not act on a single locus but on a phenotype that arises through development from a complete genotype 20 However many population genetics models of sexual species are single locus models where the fitness of an individual is calculated as the product of the contributions from each of its loci effectively assuming no epistasis In fact the genotype to fitness landscape is more complex Population genetics must either model this complexity in detail or capture it by some simpler average rule Empirically beneficial mutations tend to have a smaller fitness benefit when added to a genetic background that already has high fitness this is known as diminishing returns epistasis 21 When deleterious mutations also have a smaller fitness effect on high fitness backgrounds this is known as synergistic epistasis However the effect of deleterious mutations tends on average to be very close to multiplicative or can even show the opposite pattern known as antagonistic epistasis 22 Synergistic epistasis is central to some theories of the purging of mutation load 23 and to the evolution of sexual reproduction Mutation Edit Main article Mutation Drosophila melanogaster Mutation is the ultimate source of genetic variation in the form of new alleles In addition mutation may influence the direction of evolution when there is mutation bias i e different probabilities for different mutations to occur For example recurrent mutation that tends to be in the opposite direction to selection can lead to mutation selection balance At the molecular level if mutation from G to A happens more often than mutation from A to G then genotypes with A will tend to evolve 24 Different insertion vs deletion mutation biases in different taxa can lead to the evolution of different genome sizes 25 26 Developmental or mutational biases have also been observed in morphological evolution 27 28 For example according to the phenotype first theory of evolution mutations can eventually cause the genetic assimilation of traits that were previously induced by the environment 29 30 Mutation bias effects are superimposed on other processes If selection would favor either one out of two mutations but there is no extra advantage to having both then the mutation that occurs the most frequently is the one that is most likely to become fixed in a population 31 32 Mutation can have no effect alter the product of a gene or prevent the gene from functioning Studies in the fly Drosophila melanogaster suggest that if a mutation changes a protein produced by a gene this will probably be harmful with about 70 percent of these mutations having damaging effects and the remainder being either neutral or weakly beneficial 33 Most loss of function mutations are selected against But when selection is weak mutation bias towards loss of function can affect evolution 34 For example pigments are no longer useful when animals live in the darkness of caves and tend to be lost 35 This kind of loss of function can occur because of mutation bias and or because the function had a cost and once the benefit of the function disappeared natural selection leads to the loss Loss of sporulation ability in a bacterium during laboratory evolution appears to have been caused by mutation bias rather than natural selection against the cost of maintaining sporulation ability 36 When there is no selection for loss of function the speed at which loss evolves depends more on the mutation rate than it does on the effective population size 37 indicating that it is driven more by mutation bias than by genetic drift Mutations can involve large sections of DNA becoming duplicated usually through genetic recombination 38 This leads to copy number variation within a population Duplications are a major source of raw material for evolving new genes 39 Other types of mutation occasionally create new genes from previously noncoding DNA 40 41 Genetic drift Edit Main article Genetic drift Genetic drift is a change in allele frequencies caused by random sampling 42 That is the alleles in the offspring are a random sample of those in the parents 43 Genetic drift may cause gene variants to disappear completely and thereby reduce genetic variability In contrast to natural selection which makes gene variants more common or less common depending on their reproductive success 44 the changes due to genetic drift are not driven by environmental or adaptive pressures and are equally likely to make an allele more common as less common The effect of genetic drift is larger for alleles present in few copies than when an allele is present in many copies The population genetics of genetic drift are described using either branching processes or a diffusion equation describing changes in allele frequency 45 These approaches are usually applied to the Wright Fisher and Moran models of population genetics Assuming genetic drift is the only evolutionary force acting on an allele after t generations in many replicated populations starting with allele frequencies of p and q the variance in allele frequency across those populations is V t p q 1 exp t 2 N e displaystyle V t approx pq left 1 exp left frac t 2N e right right 46 Ronald Fisher held the view that genetic drift plays at the most a minor role in evolution and this remained the dominant view for several decades No population genetics perspective have ever given genetic drift a central role by itself but some have made genetic drift important in combination with another non selective force The shifting balance theory of Sewall Wright held that the combination of population structure and genetic drift was important Motoo Kimura s neutral theory of molecular evolution claims that most genetic differences within and between populations are caused by the combination of neutral mutations and genetic drift 47 The role of genetic drift by means of sampling error in evolution has been criticized by John H Gillespie 48 and Will Provine 49 who argue that selection on linked sites is a more important stochastic force doing the work traditionally ascribed to genetic drift by means of sampling error The mathematical properties of genetic draft are different from those of genetic drift 50 The direction of the random change in allele frequency is autocorrelated across generations 42 Gene flow Edit Gene flow is the transfer of alleles from one population to another population through immigration of individuals In this example one of the birds from population A immigrates to population B which has fewer of the dominant alleles and through mating incorporates its alleles into the other population Main article Gene flow Because of physical barriers to migration along with the limited tendency for individuals to move or spread vagility and tendency to remain or come back to natal place philopatry natural populations rarely all interbreed as may be assumed in theoretical random models panmixy 51 There is usually a geographic range within which individuals are more closely related to one another than those randomly selected from the general population This is described as the extent to which a population is genetically structured 52 The Great Wall of China is an obstacle to gene flow of some terrestrial species 53 Genetic structuring can be caused by migration due to historical climate change species range expansion or current availability of habitat Gene flow is hindered by mountain ranges oceans and deserts or even man made structures such as the Great Wall of China which has hindered the flow of plant genes 53 Gene flow is the exchange of genes between populations or species breaking down the structure Examples of gene flow within a species include the migration and then breeding of organisms or the exchange of pollen Gene transfer between species includes the formation of hybrid organisms and horizontal gene transfer Population genetic models can be used to identify which populations show significant genetic isolation from one another and to reconstruct their history 54 Subjecting a population to isolation leads to inbreeding depression Migration into a population can introduce new genetic variants 55 potentially contributing to evolutionary rescue If a significant proportion of individuals or gametes migrate it can also change allele frequencies e g giving rise to migration load 56 In the presence of gene flow other barriers to hybridization between two diverging populations of an outcrossing species are required for the populations to become new species Horizontal gene transfer Edit Current tree of life showing vertical and horizontal gene transfers Main article Horizontal gene transfer Horizontal gene transfer is the transfer of genetic material from one organism to another organism that is not its offspring this is most common among prokaryotes 57 In medicine this contributes to the spread of antibiotic resistance as when one bacteria acquires resistance genes it can rapidly transfer them to other species 58 Horizontal transfer of genes from bacteria to eukaryotes such as the yeast Saccharomyces cerevisiae and the adzuki bean beetle Callosobruchus chinensis may also have occurred 59 60 An example of larger scale transfers are the eukaryotic bdelloid rotifers which appear to have received a range of genes from bacteria fungi and plants 61 Viruses can also carry DNA between organisms allowing transfer of genes even across biological domains 62 Large scale gene transfer has also occurred between the ancestors of eukaryotic cells and prokaryotes during the acquisition of chloroplasts and mitochondria 63 Linkage EditIf all genes are in linkage equilibrium the effect of an allele at one locus can be averaged across the gene pool at other loci In reality one allele is frequently found in linkage disequilibrium with genes at other loci especially with genes located nearby on the same chromosome Recombination breaks up this linkage disequilibrium too slowly to avoid genetic hitchhiking where an allele at one locus rises to high frequency because it is linked to an allele under selection at a nearby locus Linkage also slows down the rate of adaptation even in sexual populations 64 65 66 The effect of linkage disequilibrium in slowing down the rate of adaptive evolution arises from a combination of the Hill Robertson effect delays in bringing beneficial mutations together and background selection delays in separating beneficial mutations from deleterious hitchhikers Linkage is a problem for population genetic models that treat one gene locus at a time It can however be exploited as a method for detecting the action of natural selection via selective sweeps In the extreme case of an asexual population linkage is complete and population genetic equations can be derived and solved in terms of a travelling wave of genotype frequencies along a simple fitness landscape 67 Most microbes such as bacteria are asexual The population genetics of their adaptation have two contrasting regimes When the product of the beneficial mutation rate and population size is small asexual populations follow a successional regime of origin fixation dynamics with adaptation rate strongly dependent on this product When the product is much larger asexual populations follow a concurrent mutations regime with adaptation rate less dependent on the product characterized by clonal interference and the appearance of a new beneficial mutation before the last one has fixed Applications EditExplaining levels of genetic variation Edit Neutral theory predicts that the level of nucleotide diversity in a population will be proportional to the product of the population size and the neutral mutation rate The fact that levels of genetic diversity vary much less than population sizes do is known as the paradox of variation 68 While high levels of genetic diversity were one of the original arguments in favor of neutral theory the paradox of variation has been one of the strongest arguments against neutral theory It is clear that levels of genetic diversity vary greatly within a species as a function of local recombination rate due to both genetic hitchhiking and background selection Most current solutions to the paradox of variation invoke some level of selection at linked sites 69 For example one analysis suggests that larger populations have more selective sweeps which remove more neutral genetic diversity 70 A negative correlation between mutation rate and population size may also contribute 71 Life history affects genetic diversity more than population history does e g r strategists have more genetic diversity 69 Detecting selection Edit Population genetics models are used to infer which genes are undergoing selection One common approach is to look for regions of high linkage disequilibrium and low genetic variance along the chromosome to detect recent selective sweeps A second common approach is the McDonald Kreitman test which compares the amount of variation within a species polymorphism to the divergence between species substitutions at two types of sites one assumed to be neutral Typically synonymous sites are assumed to be neutral 72 Genes undergoing positive selection have an excess of divergent sites relative to polymorphic sites The test can also be used to obtain a genome wide estimate of the proportion of substitutions that are fixed by positive selection a 73 74 According to the neutral theory of molecular evolution this number should be near zero High numbers have therefore been interpreted as a genome wide falsification of neutral theory 75 Demographic inference Edit The simplest test for population structure in a sexually reproducing diploid species is to see whether genotype frequencies follow Hardy Weinberg proportions as a function of allele frequencies For example in the simplest case of a single locus with two alleles denoted A and a at frequencies p and q random mating predicts freq AA p2 for the AA homozygotes freq aa q2 for the aa homozygotes and freq Aa 2pq for the heterozygotes In the absence of population structure Hardy Weinberg proportions are reached within 1 2 generations of random mating More typically there is an excess of homozygotes indicative of population structure The extent of this excess can be quantified as the inbreeding coefficient F Individuals can be clustered into K subpopulations 76 77 The degree of population structure can then be calculated using FST which is a measure of the proportion of genetic variance that can be explained by population structure Genetic population structure can then be related to geographic structure and genetic admixture can be detected Coalescent theory relates genetic diversity in a sample to demographic history of the population from which it was taken It normally assumes neutrality and so sequences from more neutrally evolving portions of genomes are therefore selected for such analyses It can be used to infer the relationships between species phylogenetics as well as the population structure demographic history e g population bottlenecks population growth biological dispersal source sink dynamics 78 and introgression within a species Another approach to demographic inference relies on the allele frequency spectrum 79 Evolution of genetic systems Edit By assuming that there are loci that control the genetic system itself population genetic models are created to describe the evolution of dominance and other forms of robustness the evolution of sexual reproduction and recombination rates the evolution of mutation rates the evolution of evolutionary capacitors the evolution of costly signalling traits the evolution of ageing and the evolution of co operation For example most mutations are deleterious so the optimal mutation rate for a species may be a trade off between the damage from a high deleterious mutation rate and the metabolic costs of maintaining systems to reduce the mutation rate such as DNA repair enzymes 80 One important aspect of such models is that selection is only strong enough to purge deleterious mutations and hence overpower mutational bias towards degradation if the selection coefficient s is greater than the inverse of the effective population size This is known as the drift barrier and is related to the nearly neutral theory of molecular evolution Drift barrier theory predicts that species with large effective population sizes will have highly streamlined efficient genetic systems while those with small population sizes will have bloated and complex genomes containing for example introns and transposable elements 81 However somewhat paradoxically species with large population sizes might be so tolerant to the consequences of certain types of errors that they evolve higher error rates e g in transcription and translation than small populations 82 See also EditGenotype phenotype distinction Haldane s dilemma Human genetic variation Laboratory experiments of speciation List of population genetics projects Muller s ratchet Viral quasispeciesReferences Edit Population genetics Latest research and news www nature com Retrieved 2018 01 29 Servedio Maria R Brandvain Yaniv Dhole Sumit Fitzpatrick Courtney L Goldberg Emma E Stern Caitlin A Van Cleve Jeremy Yeh D Justin 9 December 2014 Not Just a Theory The Utility of Mathematical Models in Evolutionary Biology PLOS Biology 12 12 e1002017 doi 10 1371 journal pbio 1002017 PMC 4260780 PMID 25489940 Ewens W J 2004 Mathematical Population Genetics 2nd ed New York Springer ISBN 978 0 387 20191 7 a b c Bowler Peter J 2003 Evolution the history of an idea 3rd ed Berkeley University of California Press pp 325 339 ISBN 978 0 520 23693 6 a b c Larson Edward J 2004 Evolution the remarkable history of a scientific theory Modern Library ed New York Modern Library pp 221 243 ISBN 978 0 679 64288 6 Beatty John 1986 The Synthesis and the Synthetic Theory Integrating Scientific Disciplines Science and Philosophy Vol 2 Springer Netherlands pp 125 135 doi 10 1007 978 94 010 9435 1 7 ISBN 9789024733422 Mayr Ernst Provine William B eds 1998 The Evolutionary synthesis perspectives on the unification of biology New ed ed Cambridge Massachusetts Harvard University Press pp 295 298 ISBN 9780674272262 a b Provine W B 1988 Progress in evolution and meaning in life Evolutionary progress University of Chicago Press pp 49 79 a b Provine William B 1978 The role of mathematical population geneticists in the evolutionary synthesis of the 1930s and 1940s Studies of the History of Biology 2 167 192 PMID 11610409 Ford E B 1975 1964 Ecological genetics 4th ed London Chapman and Hall pp 1ff Mayr Ernst 1988 Toward a New Philosophy of Biology Observations of an Evolutionist Cambridge Massachusetts Belknap Press of Harvard University Press p 402 ISBN 978 0 674 89665 9 Mayr Ernst Provine William B eds 1998 The Evolutionary Synthesis perspectives on the unification of biology New ed ed Cambridge Massachusetts Harvard University Press pp 338 341 ISBN 9780674272262 a b c McCandlish David M Stoltzfus Arlin September 2014 Modeling Evolution Using the Probability of Fixation History and Implications The Quarterly Review of Biology 89 3 225 252 doi 10 1086 677571 PMID 25195318 S2CID 19619966 Crow James F 2010 Wright and Fisher on Inbreeding and Random Drift Genetics 184 3 609 611 doi 10 1534 genetics 109 110023 ISSN 0016 6731 PMC 2845331 PMID 20332416 Casillas Sonia Barbadilla Antonio 2017 Molecular Population Genetics Genetics 205 3 1003 1035 doi 10 1534 genetics 116 196493 PMC 5340319 PMID 28270526 Haldane J B S 1927 A Mathematical Theory of Natural and Artificial Selection Part V Selection and Mutation Mathematical Proceedings of the Cambridge Philosophical Society 23 7 838 844 Bibcode 1927PCPS 23 838H doi 10 1017 S0305004100015644 S2CID 86716613 Orr H A 2010 The population genetics of beneficial mutations Philosophical Transactions of the Royal Society B Biological Sciences 365 1544 1195 1201 doi 10 1098 rstb 2009 0282 PMC 2871816 PMID 20308094 Hermisson J Pennings P S 2005 Soft sweeps molecular population genetics of adaptation from standing genetic variation Genetics 169 4 2335 2352 doi 10 1534 genetics 104 036947 PMC 1449620 PMID 15716498 Gillespie John 2004 Population Genetics A Concise Guide 2nd ed Johns Hopkins University Press ISBN 978 0 8018 8008 7 Miko I 2008 Epistasis Gene interaction and phenotype effects Nature Education 1 1 197 Berger D Postma E 13 October 2014 Biased Estimates of Diminishing Returns Epistasis Empirical Evidence Revisited Genetics 198 4 1417 1420 doi 10 1534 genetics 114 169870 PMC 4256761 PMID 25313131 Kouyos Roger D Silander Olin K Bonhoeffer Sebastian June 2007 Epistasis between deleterious mutations and the evolution of recombination Trends in Ecology amp Evolution 22 6 308 315 doi 10 1016 j tree 2007 02 014 PMID 17337087 Crow J F 5 August 1997 The high spontaneous mutation rate is it a health risk Proceedings of the National Academy of Sciences of the United States of America 94 16 8380 8386 Bibcode 1997PNAS 94 8380C doi 10 1073 pnas 94 16 8380 PMC 33757 PMID 9237985 Smith N G C Webster M T Ellegren H 2002 Deterministic Mutation Rate Variation in the Human Genome Genome Research 12 9 1350 1356 doi 10 1101 gr 220502 PMC 186654 PMID 12213772 Petrov D A 2000 Evidence for DNA Loss as a Determinant of Genome Size Science 287 5455 1060 1062 Bibcode 2000Sci 287 1060P doi 10 1126 science 287 5455 1060 ISSN 0036 8075 PMID 10669421 Petrov D A 2002 DNA loss and evolution of genome size in Drosophila Genetica 115 1 81 91 doi 10 1023 A 1016076215168 PMID 12188050 S2CID 5314242 Kiontke K Barriere A Kolotuev I Podbilewicz B Sommer R Fitch D H A Felix M A 2007 Trends stasis and drift in the evolution of nematode vulva development Current Biology 17 22 1925 1937 doi 10 1016 j cub 2007 10 061 PMID 18024125 S2CID 4503181 Braendle C Baer C F Felix M A 2010 Barsh Gregory S ed Bias and Evolution of the Mutationally Accessible Phenotypic Space in a Developmental System PLOS Genetics 6 3 e1000877 doi 10 1371 journal pgen 1000877 PMC 2837400 PMID 20300655 Palmer RA 2004 Symmetry breaking and the evolution of development Science 306 5697 828 833 Bibcode 2004Sci 306 828P CiteSeerX 10 1 1 631 4256 doi 10 1126 science 1103707 PMID 15514148 S2CID 32054147 West Eberhard M J 2003 Developmental plasticity and evolution New York Oxford University Press ISBN 978 0 19 512235 0 Stoltzfus A Yampolsky L Y 2009 Climbing Mount Probable Mutation as a Cause of Nonrandomness in Evolution Journal of Heredity 100 5 637 647 doi 10 1093 jhered esp048 PMID 19625453 Yampolsky L Y Stoltzfus A 2001 Bias in the introduction of variation as an orienting factor in evolution Evol Dev 3 2 73 83 doi 10 1046 j 1525 142x 2001 003002073 x PMID 11341676 S2CID 26956345 Sawyer S A Parsch J Zhang Z Hartl D L 2007 Prevalence of positive selection among nearly neutral amino acid replacements in Drosophila Proceedings of the National Academy of Sciences 104 16 6504 6510 doi 10 1073 pnas 0701572104 ISSN 0027 8424 PMC 1871816 PMID 17409186 Haldane J B S 1933 The Part Played by Recurrent Mutation in Evolution American Naturalist 67 708 5 19 doi 10 1086 280465 JSTOR 2457127 S2CID 84059440 Protas Meredith Conrad M Gross J B Tabin C Borowsky R 2007 Regressive evolution in the Mexican cave tetra Astyanax mexicanus Current Biology 17 5 452 454 doi 10 1016 j cub 2007 01 051 PMC 2570642 PMID 17306543 Maughan H Masel J Birky W C Nicholson W L 2007 The roles of mutation accumulation and selection in loss of sporulation in experimental populations of Bacillus subtilis Genetics 177 2 937 948 doi 10 1534 genetics 107 075663 PMC 2034656 PMID 17720926 Masel J King O D Maughan H 2007 The loss of adaptive plasticity during long periods of environmental stasis American Naturalist 169 1 38 46 doi 10 1086 510212 PMC 1766558 PMID 17206583 Hastings P J Lupski J R Rosenberg S M Ira G 2009 Mechanisms of change in gene copy number Nature Reviews Genetics 10 8 551 564 doi 10 1038 nrg2593 PMC 2864001 PMID 19597530 M Long Betran E Thornton K Wang W November 2003 The origin of new genes glimpses from the young and old Nat Rev Genet 4 11 865 75 doi 10 1038 nrg1204 PMID 14634634 S2CID 33999892 Liu N Okamura K Tyler D M Phillips Chung Lai 2008 The evolution and functional diversification of animal microRNA genes Cell Research 18 10 985 996 doi 10 1038 cr 2008 278 PMC 2712117 PMID 18711447 McLysaght Aoife Hurst Laurence D 25 July 2016 Open questions in the study of de novo genes what how and why Nature Reviews Genetics 17 9 567 578 doi 10 1038 nrg 2016 78 PMID 27452112 S2CID 6033249 a b Masel J 2011 Genetic drift Current Biology 21 20 R837 R838 doi 10 1016 j cub 2011 08 007 PMID 22032182 Futuyma Douglas 1998 Evolutionary Biology Sinauer Associates p Glossary ISBN 978 0 87893 189 7 Avers Charlotte 1989 Process and Pattern in Evolution Oxford University Press Wahl L M 2011 Fixation when N and s Vary Classic Approaches Give Elegant New Results Genetics 188 4 783 785 doi 10 1534 genetics 111 131748 PMC 3176088 PMID 21828279 Barton Nicholas H Briggs Derek E G Eisen Jonathan A Goldstein David B Patel Nipam H 2007 Evolution Cold Spring Harbor Laboratory Press p 417 ISBN 978 0 87969 684 9 Futuyma Douglas 1998 Evolutionary Biology Sinauer Associates p 320 ISBN 978 0 87893 189 7 Gillespie J H 2000 Genetic Drift in an Infinite Population The Pseudohitchhiking Model Genetics 155 2 909 919 doi 10 1093 genetics 155 2 909 PMC 1461093 PMID 10835409 Provine William B The Random Genetic Drift Fallacy CreateSpace Neher Richard A Shraiman Boris I August 2011 Genetic Draft and Quasi Neutrality in Large Facultatively Sexual Populations Genetics 188 4 975 996 arXiv 1108 1635 doi 10 1534 genetics 111 128876 ISSN 0016 6731 PMC 3176096 PMID 21625002 Buston P M Pilkington J G et al 2007 Are clownfish groups composed of close relatives An analysis of microsatellite DNA vraiation in Amphiprion percula Molecular Ecology 12 3 733 742 doi 10 1046 j 1365 294X 2003 01762 x PMID 12675828 S2CID 35546810 Repaci V Stow A J Briscoe D A 2007 Fine scale genetic structure co founding and multiple mating in the Australian allodapine bee Ramphocinclus brachyurus Journal of Zoology 270 4 687 691 doi 10 1111 j 1469 7998 2006 00191 x a b Su H Qu L J He K Zhang Z Wang J Chen Z Gu H 2003 The Great Wall of China a physical barrier to gene flow Heredity 90 3 212 219 doi 10 1038 sj hdy 6800237 ISSN 0018 067X PMID 12634804 S2CID 13367320 Gravel S 2012 Population Genetics Models of Local Ancestry Genetics 1202 2 607 619 arXiv 1202 4811 Bibcode 2012arXiv1202 4811G doi 10 1534 genetics 112 139808 PMC 3374321 PMID 22491189 Morjan C Rieseberg L 2004 How species evolve collectively implications of gene flow and selection for the spread of advantageous alleles Molecular Ecology 13 6 1341 56 doi 10 1111 j 1365 294X 2004 02164 x PMC 2600545 PMID 15140081 Bolnick Daniel I Nosil Patrik September 2007 Natural Selection in Populations Subject to a Migration Load Evolution 61 9 2229 2243 doi 10 1111 j 1558 5646 2007 00179 x PMID 17767592 S2CID 25685919 Boucher Yan Douady Christophe J Papke R Thane Walsh David A Boudreau Mary Ellen R Nesbo Camilla L Case Rebecca J Doolittle W Ford 2003 Lateral Gene Transfer and the Origins of Prokaryotic Groups Annual Review of Genetics 37 1 283 328 doi 10 1146 annurev genet 37 050503 084247 ISSN 0066 4197 PMID 14616063 Walsh T 2006 Combinatorial genetic evolution of multiresistance Current Opinion in Microbiology 9 5 476 82 doi 10 1016 j mib 2006 08 009 PMID 16942901 Kondo N Nikoh N Ijichi N Shimada M Fukatsu T 2002 Genome fragment of Wolbachia endosymbiont transferred to X chromosome of host insect Proceedings of the National Academy of Sciences 99 22 14280 14285 Bibcode 2002PNAS 9914280K doi 10 1073 pnas 222228199 ISSN 0027 8424 PMC 137875 PMID 12386340 Sprague G 1991 Genetic exchange between kingdoms Current Opinion in Genetics amp Development 1 4 530 533 doi 10 1016 S0959 437X 05 80203 5 PMID 1822285 Gladyshev E A Meselson M Arkhipova I R 2008 Massive Horizontal Gene Transfer in Bdelloid Rotifers Science 320 5880 1210 1213 Bibcode 2008Sci 320 1210G doi 10 1126 science 1156407 ISSN 0036 8075 PMID 18511688 S2CID 11862013 Baldo A McClure M 1 September 1999 Evolution and horizontal transfer of dUTPase encoding genes in viruses and their hosts Journal of Virology 73 9 7710 7721 doi 10 1128 JVI 73 9 7710 7721 1999 PMC 104298 PMID 10438861 Poole A Penny D 2007 Evaluating hypotheses for the origin of eukaryotes BioEssays 29 1 74 84 doi 10 1002 bies 20516 PMID 17187354 Weissman D B Hallatschek O 15 January 2014 The Rate of Adaptation in Large Sexual Populations with Linear Chromosomes Genetics 196 4 1167 1183 doi 10 1534 genetics 113 160705 PMC 3982688 PMID 24429280 Weissman Daniel B Barton Nicholas H McVean Gil 7 June 2012 Limits to the Rate of Adaptive Substitution in Sexual Populations PLOS Genetics 8 6 e1002740 doi 10 1371 journal pgen 1002740 PMC 3369949 PMID 22685419 Neher R A Shraiman B I Fisher D S 30 November 2009 Rate of Adaptation in Large Sexual Populations Genetics 184 2 467 481 arXiv 1108 3464 doi 10 1534 genetics 109 109009 PMC 2828726 PMID 19948891 Desai Michael M Fisher Daniel S 2007 Beneficial Mutation Selection Balance and the Effect of Linkage on Positive Selection Genetics 176 3 1759 1798 doi 10 1534 genetics 106 067678 PMC 1931526 PMID 17483432 Lewontin R C 1973 The genetic basis of evolutionary change 4th printing ed New York Columbia University Press ISBN 978 0231033923 a b Ellegren Hans Galtier Nicolas 6 June 2016 Determinants of genetic diversity Nature Reviews Genetics 17 7 422 433 doi 10 1038 nrg 2016 58 PMID 27265362 S2CID 23531428 Corbett Detig Russell B Hartl Daniel L Sackton Timothy B Barton Nick H 10 April 2015 Natural Selection Constrains Neutral Diversity across A Wide Range of Species PLOS Biology 13 4 e1002112 doi 10 1371 journal pbio 1002112 PMC 4393120 PMID 25859758 Sung W Ackerman M S Miller S F Doak T G Lynch M 17 October 2012 Drift barrier hypothesis and mutation rate evolution PDF Proceedings of the National Academy of Sciences 109 45 18488 18492 Bibcode 2012PNAS 10918488S doi 10 1073 pnas 1216223109 PMC 3494944 PMID 23077252 Charlesworth J Eyre Walker 2008 The McDonald Kreitman Test and Slightly Deleterious Mutations Molecular Biology and Evolution 25 6 1007 1015 doi 10 1093 molbev msn005 PMID 18195052 Eyre Walker A 2006 The genomic rate of adaptive evolution PDF Trends in Ecology and Evolution 21 10 569 575 doi 10 1016 j tree 2006 06 015 PMID 16820244 Smith N G C Eyre Walker A 2002 Adaptive protein evolution in Drosophila Nature 415 6875 1022 1024 Bibcode 2002Natur 415 1022S doi 10 1038 4151022a PMID 11875568 S2CID 4426258 Hahn M W 2008 Toward a selection theory of molecular evolution Evolution 62 2 255 265 doi 10 1111 j 1558 5646 2007 00308 x PMID 18302709 S2CID 5986211 Pritchard J K Stephens M Donnelly P June 2000 Inference of population structure using multilocus genotype data Genetics 155 2 945 959 doi 10 1093 genetics 155 2 945 ISSN 0016 6731 PMC 1461096 PMID 10835412 Verity Robert Nichols Richard A August 2016 Estimating the Number of Subpopulations K in Structured Populations Genetics 203 4 1827 1839 doi 10 1534 genetics 115 180992 ISSN 0016 6731 PMC 4981280 PMID 27317680 Manlik Oliver Chabanne Delphine Daniel Claire Bejder Lars Allen Simon J Sherwin William B 13 November 2018 Demography and genetics suggest reversal of dolphin source sink dynamics with implications for conservation Marine Mammal Science 35 3 732 759 doi 10 1111 mms 12555 S2CID 92108810 Gutenkunst Ryan N Hernandez Ryan D Williamson Scott H Bustamante Carlos D McVean Gil 23 October 2009 Inferring the Joint Demographic History of Multiple Populations from Multidimensional SNP Frequency Data PLOS Genetics 5 10 e1000695 arXiv 0909 0925 doi 10 1371 journal pgen 1000695 PMC 2760211 PMID 19851460 Sniegowski P 2000 Gerrish P Johnson T Shaver A The evolution of mutation rates separating causes from consequences BioEssays 22 12 1057 1066 doi 10 1002 1521 1878 200012 22 12 lt 1057 AID BIES3 gt 3 0 CO 2 W PMID 11084621 S2CID 36771934 Lynch Michael Conery John S 2003 The origins of genome complexity Science 302 5649 1401 1404 Bibcode 2003Sci 302 1401L CiteSeerX 10 1 1 135 974 doi 10 1126 science 1089370 PMID 14631042 S2CID 11246091 Rajon E Masel J 3 January 2011 Evolution of molecular error rates and the consequences for evolvability Proceedings of the National Academy of Sciences 108 3 1082 1087 Bibcode 2011PNAS 108 1082R doi 10 1073 pnas 1012918108 PMC 3024668 PMID 21199946 External links Edit Wikimedia Commons has media related to Population genetics Population Genetics Tutorials Molecular population genetics The ALlele FREquency Database at Yale University EHSTRAFD org Earth Human STR Allele Frequencies Database History of population genetics How Selection Changes the Genetic Composition of Population video of lecture by Stephen C Stearns Yale University National Geographic Atlas of the Human Journey Haplogroup based human migration maps Portal Evolutionary biology Retrieved from https en wikipedia org w index php title Population genetics amp 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