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Mutagenesis

February 15, 2024

This article is about mutagenesis as a general process. For mutagenesis as a laboratory technique, see Mutagenesis (molecular biology technique).

Mutagenesis (/mjuːtəˈɛnɪsɪs/) is a process by which the genetic information of an organism is changed by the production of a mutation. It may occur spontaneously in nature, or as a result of exposure to mutagens. It can also be achieved experimentally using laboratory procedures. A mutagen is a mutation-causing agent, be it chemical or physical, which results in an increased rate of mutations in an organism's genetic code. In nature mutagenesis can lead to cancer and various heritable diseases, and it is also a driving force of evolution. Mutagenesis as a science was developed based on work done by Hermann Muller, Charlotte Auerbach and J. M. Robson in the first half of the 20th century.[1]

History edit

DNA may be modified, either naturally or artificially, by a number of physical, chemical and biological agents, resulting in mutations. Hermann Muller found that "high temperatures" have the ability to mutate genes in the early 1920s,[2] and in 1927, demonstrated a causal link to mutation upon experimenting with an x-ray machine, noting phylogenetic changes when irradiating fruit flies with relatively high dose of X-rays.[3][4] Muller observed a number of chromosome rearrangements in his experiments, and suggested mutation as a cause of cancer.[5][6] The association of exposure to radiation and cancer had been observed as early as 1902, six years after the discovery of X-ray by Wilhelm Röntgen, and the discovery of radioactivity by Henri Becquerel.[7] Lewis Stadler, Muller's contemporary, also showed the effect of X-rays on mutations in barley in 1928, and of ultraviolet (UV) radiation on maize in 1936.[8] In 1940s, Charlotte Auerbach and J. M. Robson found that mustard gas can also cause mutations in fruit flies.[9]

While changes to the chromosome caused by X-ray and mustard gas were readily observable to early researchers, other changes to the DNA induced by other mutagens were not so easily observable; the mechanism by which they occur may be complex, and take longer to unravel. For example, soot was suggested to be a cause of cancer as early as 1775,[10] and coal tar was demonstrated to cause cancer in 1915.[11] The chemicals involved in both were later shown to be polycyclic aromatic hydrocarbons (PAH).[12] PAHs by themselves are not carcinogenic, and it was proposed in 1950 that the carcinogenic forms of PAHs are the oxides produced as metabolites from cellular processes.[13] The metabolic process was identified in 1960s as catalysis by cytochrome P450, which produces reactive species that can interact with the DNA to form adducts, or product molecules resulting from the reaction of DNA and, in this case, cytochrome P450;[14][15] the mechanism by which the PAH adducts give rise to mutation, however, is still under investigation.

Distinction between a mutation and DNA damage edit

DNA damage is an abnormal alteration in the structure of DNA that cannot, itself, be replicated when DNA replicates. In contrast, a mutation is a change in the nucleic acid sequence that can be replicated; hence, a mutation can be inherited from one generation to the next. Damage can occur from chemical addition (adduct), or structural disruption to a base of DNA (creating an abnormal nucleotide or nucleotide fragment), or a break in one or both DNA strands. Such DNA damage may result in mutation. When DNA containing damage is replicated, an incorrect base may be inserted in the new complementary strand as it is being synthesized (see DNA repair § Translesion synthesis). The incorrect insertion in the new strand will occur opposite the damaged site in the template strand, and this incorrect insertion can become a mutation (i.e. a changed base pair) in the next round of replication. Furthermore, double-strand breaks in DNA may be repaired by an inaccurate repair process, non-homologous end joining, which produces mutations. Mutations can ordinarily be avoided if accurate DNA repair systems recognize DNA damage and repair it prior to completion of the next round of replication. At least 169 enzymes are either directly employed in DNA repair or influence DNA repair processes. Of these, 83 are directly employed in the 5 types of DNA repair processes indicated in the chart shown in the article DNA repair.

Mammalian nuclear DNA may sustain more than 60,000 damage episodes per cell per day, as listed with references in DNA damage (naturally occurring). If left uncorrected, these adducts, after misreplication past the damaged sites, can give rise to mutations. In nature, the mutations that arise may be beneficial or deleterious—this is the driving force of evolution. An organism may acquire new traits through genetic mutation, but mutation may also result in impaired function of the genes and, in severe cases, causes the death of the organism. Mutation is also a major source for acquisition of resistance to antibiotics in bacteria, and to antifungal agents in yeasts and molds.[16][17] In a laboratory setting, mutagenesis is a useful technique for generating mutations that allows the functions of genes and gene products to be examined in detail, producing proteins with improved characteristics or novel functions, as well as mutant strains with useful properties. Initially, the ability of radiation and chemical mutagens to cause mutation was exploited to generate random mutations, but later techniques were developed to introduce specific mutations.

In humans, an average of 60 new mutations are transmitted from parent to offspring. Human males, however, tend to pass on more mutations depending on their age, transmitting an average of two new mutations to their progeny with every additional year of their age.[18][19]

Mechanisms edit

Mutagenesis may occur endogenously (e.g. spontaneous hydrolysis), through normal cellular processes that can generate reactive oxygen species and DNA adducts, or through error in DNA replication and repair.[20] Mutagenesis may also occur as a result of the presence of environmental mutagens that induce changes to an organism's DNA. The mechanism by which mutation occurs varies according to the mutagen, or the causative agent, involved. Most mutagens act either directly, or indirectly via mutagenic metabolites, on an organism's DNA, producing lesions. Some mutagens, however, may affect the replication or chromosomal partition mechanism, and other cellular processes.

Mutagenesis may also be self-induced by unicellular organisms when environmental conditions are restrictive to the organism's growth, such as bacteria growing in the presence of antibiotics, yeast growing in the presence of an antifungal agent, or other unicellular organisms growing in an environment lacking in an essential nutrient [21][22][23]

Many chemical mutagens require biological activation to become mutagenic. An important group of enzymes involved in the generation of mutagenic metabolites is cytochrome P450.[24] Other enzymes that may also produce mutagenic metabolites include glutathione S-transferase and microsomal epoxide hydrolase. Mutagens that are not mutagenic by themselves but require biological activation are called promutagens.

While most mutagens produce effects that ultimately result in errors in replication, for example creating adducts that interfere with replication, some mutagens may directly affect the replication process or reduce its fidelity. Base analog such as 5-bromouracil may substitute for thymine in replication. Metals such as cadmium, chromium, and nickel can increase mutagenesis in a number of ways in addition to direct DNA damage, for example reducing the ability to repair errors, as well as producing epigenetic changes.[25]

Mutations often arise as a result of problems caused by DNA lesions during replication, resulting in errors in replication. In bacteria, extensive damage to DNA due to mutagens results in single-stranded DNA gaps during replication. This induces the SOS response, an emergency repair process that is also error-prone, thereby generating mutations. In mammalian cells, stalling of replication at damaged sites induces a number of rescue mechanisms that help bypass DNA lesions, however, this may also result in errors. The Y family of DNA polymerases specializes in DNA lesion bypass in a process termed translesion synthesis (TLS) whereby these lesion-bypass polymerases replace the stalled high-fidelity replicative DNA polymerase, transit the lesion and extend the DNA until the lesion has been passed so that normal replication can resume; these processes may be error-prone or error-free.

DNA damage and spontaneous mutation edit

The number of DNA damage episodes occurring in a mammalian cell per day is high (more than 60,000 per day). Frequent occurrence of DNA damage is likely a problem for all DNA- containing organisms, and the need to cope with DNA damage and minimize their deleterious effects is likely a fundamental problem for life.[citation needed]

Most spontaneous mutations likely arise from error-prone trans-lesion synthesis past a DNA damage site in the template strand during DNA replication. This process can overcome potentially lethal blockages, but at the cost of introducing inaccuracies in daughter DNA. The causal relationship of DNA damage to spontaneous mutation is illustrated by aerobically growing E. coli bacteria, in which 89% of spontaneously occurring base substitution mutations are caused by reactive oxygen species (ROS)-induced DNA damage.[26] In yeast, more than 60% of spontaneous single-base pair substitutions and deletions are likely caused by trans-lesion synthesis.[27]

An additional significant source of mutations in eukaryotes is the inaccurate DNA repair process non-homologous end joining, that is often employed in repair of double strand breaks.[28]

In general, it appears that the main underlying cause of spontaneous mutation is error-prone trans-lesion synthesis during DNA replication and that the error-prone non-homologous end-joining repair pathway may also be an important contributor in eukaryotes.

Spontaneous hydrolysis edit

DNA is not entirely stable in aqueous solution, and depurination of the DNA can occur. Under physiological conditions the glycosidic bond may be hydrolyzed spontaneously and 10,000 purine sites in DNA are estimated to be depurinated each day in a cell.[20] Numerous DNA repair pathways exist for DNA; however, if the apurinic site is not repaired, misincorporation of nucleotides may occur during replication. Adenine is preferentially incorporated by DNA polymerases in an apurinic site.

Cytidine may also become deaminated to uridine at one five-hundredth of the rate of depurination and can result in G to A transition. Eukaryotic cells also contain 5-methylcytosine, thought to be involved in the control of gene transcription, which can become deaminated into thymine.

Tautomerism edit

Main article: Tautomer

Tautomerization is the process by which compounds spontaneously rearrange themselves to assume their structural isomer forms. For example, the keto (C=O) forms of guanine and thymine can rearrange into their rare enol (-OH) forms, while the amino (-NH2 ) forms of adenine and cytosine can result in the rarer imino (=NH) forms. In DNA replication, tautomerization alters the base-pairing sites and can cause the improper pairing of nucleic acid bases.[29]

Modification of bases edit

Bases may be modified endogenously by normal cellular molecules. For example, DNA may be methylated by S-adenosylmethionine, thus altering the expression of the marked gene without incurring a mutation to the DNA sequence itself. Histone modification is a related process in which the histone proteins around which DNA coils can be similarly modified via methylation, phosphorylation, or acetylation; these modifications may act to alter gene expression of the local DNA, and may also act to denote locations of damaged DNA in need of repair. DNA may also be glycosylated by reducing sugars.

Many compounds, such as PAHs, aromatic amines, aflatoxin and pyrrolizidine alkaloids, may form reactive oxygen species catalyzed by cytochrome P450. These metabolites form adducts with the DNA, which can cause errors in replication, and the bulky aromatic adducts may form stable intercalation between bases and block replication. The adducts may also induce conformational changes in the DNA. Some adducts may also result in the depurination of the DNA;[30] it is, however, uncertain how significant such depurination as caused by the adducts is in generating mutation.

Alkylation and arylation of bases can cause errors in replication. Some alkylating agents such as N-Nitrosamines may require the catalytic reaction of cytochrome-P450 for the formation of a reactive alkyl cation. N7 and O6 of guanine and the N3 and N7 of adenine are most susceptible to attack. N7-guanine adducts form the bulk of DNA adducts, but they appear to be non-mutagenic. Alkylation at O6 of guanine, however, is harmful because excision repair of O6-adduct of guanine may be poor in some tissues such as the brain.[31] The O6 methylation of guanine can result in G to A transition, while O4-methylthymine can be mispaired with guanine. The type of the mutation generated, however, may be dependent on the size and type of the adduct as well as the DNA sequence.[32]

Ionizing radiation and reactive oxygen species often oxidize guanine to produce 8-oxoguanine.

See also: Epigenetics
 
Arrows indicates chromosomal breakages due to DNA damage

Backbone damage edit

Ionizing radiation may produce highly reactive free radicals that can break the bonds in the DNA. Double-stranded breakages are especially damaging and hard to repair, producing translocation and deletion of part of a chromosome. Alkylating agents like mustard gas may also cause breakages in the DNA backbone. Oxidative stress may also generate highly reactive oxygen species that can damage DNA. Incorrect repair of other damage induced by the highly reactive species can also lead to mutations.

Crosslinking edit

Main article: Crosslinking of DNA

Covalent bonds between the bases of nucleotides in DNA, be they in the same strand or opposing strands, is referred to as crosslinking of DNA; crosslinking of DNA may affect both the replication and the transcription of DNA, and it may be caused by exposure to a variety of agents. Some naturally occurring chemicals may also promote crosslinking, such as psoralens after activation by UV radiation, and nitrous acid. Interstrand cross-linking (between two strands) causes more damage, as it blocks replication and transcription and can cause chromosomal breakages and rearrangements. Some crosslinkers such as cyclophosphamide, mitomycin C and cisplatin are used as anticancer chemotherapeutic because of their high degree of toxicity to proliferating cells.

Dimerization edit

Main article: Dimer

Dimerization consists of the bonding of two monomers to form an oligomer, such as the formation of pyrimidine dimers as a result of exposure to UV radiation, which promotes the formation of a cyclobutyl ring between adjacent thymines in DNA.[33] In human skin cells, thousands of dimers may be formed in a day due to normal exposure to sunlight. DNA polymerase η may help bypass these lesions in an error-free manner;[34] however, individuals with defective DNA repair function, such as those with xeroderma pigmentosum, are sensitive to sunlight and may be prone to skin cancer.

 
Ethidium intercalated between two adenine-thymine base pairs.

Clinically, whether a tumor has formed as a direct consequence of UV radiation is discernible via DNA sequencing analysis for the characteristic context-specific dimerization pattern that occurs due to excessive exposure to sunlight.[35]

Intercalation between bases edit

Main article: Intercalation (biochemistry)

The planar structure of chemicals such as ethidium bromide and proflavine allows them to insert between bases in DNA. This insert causes the DNA's backbone to stretch and makes slippage in DNA during replication more likely to occur since the bonding between the strands is made less stable by the stretching. Forward slippage will result in deletion mutation, while reverse slippage will result in an insertion mutation. Also, the intercalation into DNA of anthracyclines such as daunorubicin and doxorubicin interferes with the functioning of the enzyme topoisomerase II, blocking replication as well as causing mitotic homologous recombination.

Insertional mutagenesis edit

Main article: Insertional mutagenesis

Transposons and viruses or retrotransposons may insert DNA sequences into coding regions or functional elements of a gene and result in inactivation of the gene.[36]

Adaptive mutagenesis mechanisms edit

Main article: Adaptive mutation

Adaptive mutagenesis has been defined as mutagenesis mechanisms that enable an organism to adapt to an environmental stress. Since the variety of environmental stresses is very broad, the mechanisms that enable it are also quite broad, as far as research on the field has shown. For instance, in bacteria, while modulation of the SOS response and endogenous prophage DNA synthesis has been shown to increase Acinetobacter baumannii resistance to ciprofloxacin.[16] Resistance mechanisms are presumed to be linked to chromosomal mutation untransferable via horizontal gene transfer in some members of family Enterobacteriaceae, such as E. coli, Salmonella spp., Klebsiella spp., and Enterobacter spp.[37] Chromosomal events, specially gene amplification, seem also to be relevant to this adaptive mutagenesis in bacteria.[38]

Research in eukaryotic cells is much scarcer, but chromosomal events seem also to be rather relevant: while an ectopic intrachromosomal recombination has been reported to be involved in acquisition of resistance to 5-fluorocytosine in Saccharomyces cerevisiae,[17] genome duplications have been found to confer resistance in S. cerevisiae to nutrient-poor environments.[21][39][40]

Laboratory applications edit

Main article: Mutagenesis (molecular biology technique)

In the laboratory, mutagenesis is a technique by which DNA mutations are deliberately engineered to produce mutant genes, proteins, or strains of organisms. Various constituents of a gene, such as its control elements and its gene product, may be mutated so that the function of a gene or protein can be examined in detail. The mutation may also produce mutant proteins with altered properties, or enhanced or novel functions that may prove to be of use commercially. Mutant strains of organisms that have practical applications, or allow the molecular basis of particular cell function to be investigated, may also be produced.

Early methods of mutagenesis produced entirely random mutations; however, modern methods of mutagenesis are capable of producing site-specific mutations. Modern laboratory techniques used to generate these mutations include:

See also edit

References edit

  1. ^ Beale, G. (1993). "The Discovery of Mustard Gas Mutagenesis by Auerbach and Robson in 1941". Genetics. 134 (2): 393–399. doi:10.1093/genetics/134.2.393. PMC 1205483. PMID 8325476.
  2. ^ Kevin M. Gleason Published: 2017-03-07. "Hermann Joseph Muller's Study of X-rays as a Mutagen, (1926-1927)".{{cite web}}: CS1 maint: numeric names: authors list (link)
  3. ^ "Genetics and Genomics Timeline 1927 Hermann J. Muller (1890-1967) demonstrates that X rays can induce mutations".
  4. ^ Muller, H. J. (1927). "Artificial Transmutation of the Gene" (PDF). Science. 66 (1699): 84–87. Bibcode:1927Sci....66...84M. doi:10.1126/science.66.1699.84. PMID 17802387.
  5. ^ Crow, J. F.; Abrahamson, S. (1997). "Seventy Years Ago: Mutation Becomes Experimental". Genetics. 147 (4): 1491–1496. doi:10.1093/genetics/147.4.1491. PMC 1208325. PMID 9409815.
  6. ^ Calabrese, E. J. (30 June 2011). (PDF). Archives of Toxicology. 85 (4): 1495–1498. doi:10.1007/s00204-011-0728-8. PMID 21717110. S2CID 4708210. Archived from the original (PDF) on 2 August 2017. Retrieved 30 December 2011.
  7. ^ Ronald L. Kathren (December 2002). "Historical Development of the Linear Nonthreshold Dose-Response Model as Applied to Radiation". University of New Hampshire Law Review. 1 (1).
  8. ^ Stadler, L. J.; G. F. Sprague (1936-10-15). "Genetic Effects of Ultra-Violet Radiation in Maize. I. Unfiltered Radiation" (PDF). Proc. Natl. Acad. Sci. U.S.A. 22 (10): 572–8. Bibcode:1936PNAS...22..572S. doi:10.1073/pnas.22.10.572. PMC 1076819. PMID 16588111. Retrieved 2007-10-11.
  9. ^ Auerbach, C.; Robson, J.M.; Carr, J.G. (March 1947). "Chemical Production of Mutations". Science. 105 (2723): 243–7. Bibcode:1947Sci...105..243A. doi:10.1126/science.105.2723.243. PMID 17769478.
  10. ^ Brown, J. R.; Thornton, J. L. (1957). "Percivall Pott (1714-1788) and Chimney Sweepers' Cancer of the Scrotum". British Journal of Industrial Medicine. 14 (1): 68–70. doi:10.1136/oem.14.1.68. PMC 1037746. PMID 13396156.
  11. ^ Yamagawa K, Ichikawa K (1915). "Experimentelle Studie ueber die Pathogenese der Epithel geschwuelste". Mitteilungen aus der Medizinischen Fakultät der Kaiserlichen Universität zu Tokyo. 15: 295–344.
  12. ^ Luch, Andreas (2005). "Nature and Nurture — Lessons from Chemical Carcinogenesis: Chemical Carcinogens — From Past to Present". Medscape.
  13. ^ Boyland E (1950). "The biological significance of metabolism of polycyclic compounds". Biochemical Society Symposium. 5: 40–54. ISSN 0067-8694. OCLC 216723160.
  14. ^ Omura, T.; Sato, R. (1962). "A new cytochrome in liver microsomes". The Journal of Biological Chemistry. 237 (4): 1375–1376. doi:10.1016/S0021-9258(18)60338-2. PMID 14482007.
  15. ^ Conney, A. H. (1982). "Induction of microsomal enzymes by foreign chemicals and carcinogenesis by polycyclic aromatic hydrocarbons: G. H. A. Clowes Memorial Lecture". Cancer Research. 42 (12): 4875–4917. PMID 6814745.
  16. ^ a b Geisinger, Edward; Vargas-Cuebas, Germán; Mortman, Nadav J.; Syal, Sapna; Dai, Yunfei; Wainwright, Elizabeth L.; Lazinski, David; Wood, Stephen; Zhu, Zeyu (2019-06-11). Miller, Samuel I. (ed.). "The Landscape of Phenotypic and Transcriptional Responses to Ciprofloxacin in Acinetobacter baumannii : Acquired Resistance Alleles Modulate Drug-Induced SOS Response and Prophage Replication". mBio. 10 (3). doi:10.1128/mBio.01127-19. ISSN 2150-7511. PMC 6561030. PMID 31186328.
  17. ^ a b Quinto-Alemany, David; Canerina-Amaro, Ana; Hernández-Abad, Luís G.; Machín, Félix; Romesberg, Floyd E.; Gil-Lamaignere, Cristina (2012-07-31). Sturtevant, Joy (ed.). "Yeasts Acquire Resistance Secondary to Antifungal Drug Treatment by Adaptive Mutagenesis". PLOS ONE. 7 (7): e42279. Bibcode:2012PLoSO...742279Q. doi:10.1371/journal.pone.0042279. ISSN 1932-6203. PMC 3409178. PMID 22860105.
  18. ^ Jha, Alok (22 August 2012). "Older fathers pass on more genetic mutations, study shows". The Guardian.
  19. ^ Kong, A.; Frigge, M. L.; Masson, G.; Besenbacher, S.; Sulem, P.; Magnusson, G.; Gudjonsson, S. A.; Sigurdsson, A.; Jonasdottir, A.; Jonasdottir, A.; Wong, W. S.; Sigurdsson, G.; Walters, G. B.; Steinberg, S.; Helgason, H.; Thorleifsson, G.; Gudbjartsson, D. F.; Helgason, A.; Magnusson, O. T.; Thorsteinsdottir, U.; Stefansson, K. (2012). "Rate of de novo mutations and the importance of father's age to disease risk". Nature. 488 (7412): 471–475. Bibcode:2012Natur.488..471K. doi:10.1038/nature11396. PMC 3548427. PMID 22914163.
  20. ^ a b Loeb, L. A. (1989). "Endogenous carcinogenesis: Molecular oncology into the twenty-first century--presidential address" (PDF). Cancer Research. 49 (20): 5489–5496. PMID 2676144.
  21. ^ a b Heidenreich, Erich (January 2007). "Adaptive Mutation in Saccharomyces cerevisiae". Critical Reviews in Biochemistry and Molecular Biology. 42 (4): 285–311. doi:10.1080/10409230701507773. ISSN 1040-9238. PMID 17687670. S2CID 11594730.
  22. ^ Quinto-Alemany, David; Canerina-Amaro, Ana; Hernández-Abad, Luís G.; Machín, Félix; Romesberg, Floyd E.; Gil-Lamaignere, Cristina (2012-07-31). Sturtevant, Joy (ed.). "Yeasts Acquire Resistance Secondary to Antifungal Drug Treatment by Adaptive Mutagenesis". PLOS ONE. 7 (7): e42279. Bibcode:2012PLoSO...742279Q. doi:10.1371/journal.pone.0042279. ISSN 1932-6203. PMC 3409178. PMID 22860105.
  23. ^ Aghapour, Zahra; Gholizadeh, Pourya; Ganbarov, Khudaverdi; bialvaei, Abed Zahedi; Mahmood, Suhad Saad; Tanomand, Asghar; Yousefi, Mehdi; Asgharzadeh, Mohammad; Yousefi, Bahman (April 2019). "Molecular mechanisms related to colistin resistance in Enterobacteriaceae". Infection and Drug Resistance. 12: 965–975. doi:10.2147/idr.s199844. PMC 6519339. PMID 31190901.
  24. ^ Trevor M. Penning (2011). Chemical Carcinogenesis (Current Cancer Research). Springer. ISBN 978-1617379949.
  25. ^ Salnikow K, Zhitkovich (January 2008). "Genetic and epigenetic mechanisms in metal carcinogenesis and cocarcinogenesis: nickel, arsenic, and chromium". Chemical Research in Toxicology. 21 (1): 28–44. doi:10.1021/tx700198a. PMC 2602826. PMID 17970581.
  26. ^ Sakai A, Nakanishi M, Yoshiyama K, Maki H (July 2006). "Impact of reactive oxygen species on spontaneous mutagenesis in Escherichia coli". Genes Cells. 11 (7): 767–78. doi:10.1111/j.1365-2443.2006.00982.x. PMID 16824196. S2CID 1365658.
  27. ^ Kunz BA, Ramachandran K, Vonarx EJ (April 1998). "DNA sequence analysis of spontaneous mutagenesis in Saccharomyces cerevisiae". Genetics. 148 (4): 1491–505. doi:10.1093/genetics/148.4.1491. PMC 1460101. PMID 9560369.
  28. ^ Huertas P (January 2010). "DNA resection in eukaryotes: deciding how to fix the break". Nat. Struct. Mol. Biol. 17 (1): 11–6. doi:10.1038/nsmb.1710. PMC 2850169. PMID 20051983.
  29. ^ Sinden, Richard R. (1994). DNA Structure and Function. Academic Press. pp. 17–20. ISBN 978-0126457506.
  30. ^ Melendez-Colon, V. J.; Smith, C. A.; Seidel, A.; Luch, A.; Platt, K. L.; Baird, W. M. (1997). "Formation of stable adducts and absence of depurinating DNA adducts in cells and DNA treated with the potent carcinogen dibenzoa, lpyrene or its diol epoxides". Proceedings of the National Academy of Sciences of the United States of America. 94 (25): 13542–13547. Bibcode:1997PNAS...9413542M. doi:10.1073/pnas.94.25.13542. PMC 28342. PMID 9391062.
  31. ^ Boysen, G.; Pachkowski, B. F.; Nakamura, J.; Swenberg, J. A. (2009). "The Formation and Biological Significance of N7-Guanine Adducts". Mutation Research/Genetic Toxicology and Environmental Mutagenesis. 678 (2): 76–94. doi:10.1016/j.mrgentox.2009.05.006. PMC 2739241. PMID 19465146.
  32. ^ Loechler, E. L. (1996). "The role of adduct site-specific mutagenesis in understanding how carcinogen-DNA adducts cause mutations: Perspective, prospects and problems". Carcinogenesis. 17 (5): 895–902. doi:10.1093/carcin/17.5.895. PMID 8640935.
  33. ^ Setlow, R. B. (1966). "Cyclobutane-type pyrimidine dimers in polynucleotides". Science. 153 (734): 379–386. Bibcode:1966Sci...153..379S. doi:10.1126/science.153.3734.379. PMID 5328566. S2CID 11210761.
  34. ^ Broyde, S.; Patel, D. J. (2010). "DNA repair: How to accurately bypass damage". Nature. 465 (7301): 1023–1024. Bibcode:2010Natur.465.1023B. doi:10.1038/4651023a. PMC 4986998. PMID 20577203.
  35. ^ Mata, Douglas A.; Williams, Erik A.; Sokol, Ethan; Oxnard, Geoffrey R.; Fleischmann, Zoe; Tse, Julie Y.; Decker, Brennan (23 March 2022). "Prevalence of UV Mutational Signatures Among Cutaneous Primary Tumors". JAMA Network Open. 5 (3): e223833. doi:10.1001/jamanetworkopen.2022.3833. PMC 8943639. PMID 35319765.
  36. ^ Mohanasundaram, Boominathan; Rajmane, Vyankatesh B.; Jogdand, Sukanya V.; Bhide, Amey J.; Banerjee, Anjan K. (June 2019). "Agrobacterium-mediated Tnt1 mutagenesis of moss protonemal filaments and generation of stable mutants with impaired gametophyte". Molecular Genetics and Genomics. 294 (3): 583–596. doi:10.1007/s00438-019-01532-4. PMID 30689096. S2CID 59304089.
  37. ^ Aghapour, Zahra; Gholizadeh, Pourya; Ganbarov, Khudaverdi; bialvaei, Abed Zahedi; Mahmood, Suhad Saad; Tanomand, Asghar; Yousefi, Mehdi; Asgharzadeh, Mohammad; Yousefi, Bahman (April 2019). "Molecular mechanisms related to colistin resistance in Enterobacteriaceae". Infection and Drug Resistance. 12: 965–975. doi:10.2147/idr.s199844. PMC 6519339. PMID 31190901.
  38. ^ Hersh, Megan N; Ponder, Rebecca G; Hastings, P.J; Rosenberg, Susan M (June 2004). "Adaptive mutation and amplification in Escherichia coli: two pathways of genome adaptation under stress". Research in Microbiology. 155 (5): 352–359. doi:10.1016/j.resmic.2004.01.020. PMID 15207867.
  39. ^ Longerich, S.; Galloway, A. M.; Harris, R. S.; Wong, C.; Rosenberg, S. M. (1995-12-19). "Adaptive mutation sequences reproduced by mismatch repair deficiency". Proceedings of the National Academy of Sciences. 92 (26): 12017–12020. Bibcode:1995PNAS...9212017L. doi:10.1073/pnas.92.26.12017. ISSN 0027-8424. PMC 40287. PMID 8618835.
  40. ^ Rosenberg, Susan M.; Fitzgerald, Devon M. (2019-04-01). "What is mutation? A chapter in the series: How microbes "jeopardize" the modern synthesis". PLOS Genetics. 15 (4): e1007995. doi:10.1371/journal.pgen.1007995. ISSN 1553-7404. PMC 6443146. PMID 30933985.
 
Look up mutagenesis in Wiktionary, the free dictionary.

February 15, 2024
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This article is about mutagenesis as a general process For mutagenesis as a laboratory technique see Mutagenesis molecular biology technique Mutagenesis m juː t e ˈ dʒ ɛ n ɪ s ɪ s is a process by which the genetic information of an organism is changed by the production of a mutation It may occur spontaneously in nature or as a result of exposure to mutagens It can also be achieved experimentally using laboratory procedures A mutagen is a mutation causing agent be it chemical or physical which results in an increased rate of mutations in an organism s genetic code In nature mutagenesis can lead to cancer and various heritable diseases and it is also a driving force of evolution Mutagenesis as a science was developed based on work done by Hermann Muller Charlotte Auerbach and J M Robson in the first half of the 20th century 1 Contents 1 History 2 Distinction between a mutation and DNA damage 3 Mechanisms 3 1 DNA damage and spontaneous mutation 3 2 Spontaneous hydrolysis 3 3 Tautomerism 3 4 Modification of bases 3 5 Backbone damage 3 6 Crosslinking 3 7 Dimerization 3 8 Intercalation between bases 3 9 Insertional mutagenesis 3 10 Adaptive mutagenesis mechanisms 4 Laboratory applications 5 See also 6 ReferencesHistory editDNA may be modified either naturally or artificially by a number of physical chemical and biological agents resulting in mutations Hermann Muller found that high temperatures have the ability to mutate genes in the early 1920s 2 and in 1927 demonstrated a causal link to mutation upon experimenting with an x ray machine noting phylogenetic changes when irradiating fruit flies with relatively high dose of X rays 3 4 Muller observed a number of chromosome rearrangements in his experiments and suggested mutation as a cause of cancer 5 6 The association of exposure to radiation and cancer had been observed as early as 1902 six years after the discovery of X ray by Wilhelm Rontgen and the discovery of radioactivity by Henri Becquerel 7 Lewis Stadler Muller s contemporary also showed the effect of X rays on mutations in barley in 1928 and of ultraviolet UV radiation on maize in 1936 8 In 1940s Charlotte Auerbach and J M Robson found that mustard gas can also cause mutations in fruit flies 9 While changes to the chromosome caused by X ray and mustard gas were readily observable to early researchers other changes to the DNA induced by other mutagens were not so easily observable the mechanism by which they occur may be complex and take longer to unravel For example soot was suggested to be a cause of cancer as early as 1775 10 and coal tar was demonstrated to cause cancer in 1915 11 The chemicals involved in both were later shown to be polycyclic aromatic hydrocarbons PAH 12 PAHs by themselves are not carcinogenic and it was proposed in 1950 that the carcinogenic forms of PAHs are the oxides produced as metabolites from cellular processes 13 The metabolic process was identified in 1960s as catalysis by cytochrome P450 which produces reactive species that can interact with the DNA to form adducts or product molecules resulting from the reaction of DNA and in this case cytochrome P450 14 15 the mechanism by which the PAH adducts give rise to mutation however is still under investigation Distinction between a mutation and DNA damage editDNA damage is an abnormal alteration in the structure of DNA that cannot itself be replicated when DNA replicates In contrast a mutation is a change in the nucleic acid sequence that can be replicated hence a mutation can be inherited from one generation to the next Damage can occur from chemical addition adduct or structural disruption to a base of DNA creating an abnormal nucleotide or nucleotide fragment or a break in one or both DNA strands Such DNA damage may result in mutation When DNA containing damage is replicated an incorrect base may be inserted in the new complementary strand as it is being synthesized see DNA repair Translesion synthesis The incorrect insertion in the new strand will occur opposite the damaged site in the template strand and this incorrect insertion can become a mutation i e a changed base pair in the next round of replication Furthermore double strand breaks in DNA may be repaired by an inaccurate repair process non homologous end joining which produces mutations Mutations can ordinarily be avoided if accurate DNA repair systems recognize DNA damage and repair it prior to completion of the next round of replication At least 169 enzymes are either directly employed in DNA repair or influence DNA repair processes Of these 83 are directly employed in the 5 types of DNA repair processes indicated in the chart shown in the article DNA repair Mammalian nuclear DNA may sustain more than 60 000 damage episodes per cell per day as listed with references in DNA damage naturally occurring If left uncorrected these adducts after misreplication past the damaged sites can give rise to mutations In nature the mutations that arise may be beneficial or deleterious this is the driving force of evolution An organism may acquire new traits through genetic mutation but mutation may also result in impaired function of the genes and in severe cases causes the death of the organism Mutation is also a major source for acquisition of resistance to antibiotics in bacteria and to antifungal agents in yeasts and molds 16 17 In a laboratory setting mutagenesis is a useful technique for generating mutations that allows the functions of genes and gene products to be examined in detail producing proteins with improved characteristics or novel functions as well as mutant strains with useful properties Initially the ability of radiation and chemical mutagens to cause mutation was exploited to generate random mutations but later techniques were developed to introduce specific mutations In humans an average of 60 new mutations are transmitted from parent to offspring Human males however tend to pass on more mutations depending on their age transmitting an average of two new mutations to their progeny with every additional year of their age 18 19 Mechanisms editMutagenesis may occur endogenously e g spontaneous hydrolysis through normal cellular processes that can generate reactive oxygen species and DNA adducts or through error in DNA replication and repair 20 Mutagenesis may also occur as a result of the presence of environmental mutagens that induce changes to an organism s DNA The mechanism by which mutation occurs varies according to the mutagen or the causative agent involved Most mutagens act either directly or indirectly via mutagenic metabolites on an organism s DNA producing lesions Some mutagens however may affect the replication or chromosomal partition mechanism and other cellular processes Mutagenesis may also be self induced by unicellular organisms when environmental conditions are restrictive to the organism s growth such as bacteria growing in the presence of antibiotics yeast growing in the presence of an antifungal agent or other unicellular organisms growing in an environment lacking in an essential nutrient 21 22 23 Many chemical mutagens require biological activation to become mutagenic An important group of enzymes involved in the generation of mutagenic metabolites is cytochrome P450 24 Other enzymes that may also produce mutagenic metabolites include glutathione S transferase and microsomal epoxide hydrolase Mutagens that are not mutagenic by themselves but require biological activation are called promutagens While most mutagens produce effects that ultimately result in errors in replication for example creating adducts that interfere with replication some mutagens may directly affect the replication process or reduce its fidelity Base analog such as 5 bromouracil may substitute for thymine in replication Metals such as cadmium chromium and nickel can increase mutagenesis in a number of ways in addition to direct DNA damage for example reducing the ability to repair errors as well as producing epigenetic changes 25 Mutations often arise as a result of problems caused by DNA lesions during replication resulting in errors in replication In bacteria extensive damage to DNA due to mutagens results in single stranded DNA gaps during replication This induces the SOS response an emergency repair process that is also error prone thereby generating mutations In mammalian cells stalling of replication at damaged sites induces a number of rescue mechanisms that help bypass DNA lesions however this may also result in errors The Y family of DNA polymerases specializes in DNA lesion bypass in a process termed translesion synthesis TLS whereby these lesion bypass polymerases replace the stalled high fidelity replicative DNA polymerase transit the lesion and extend the DNA until the lesion has been passed so that normal replication can resume these processes may be error prone or error free DNA damage and spontaneous mutation edit The number of DNA damage episodes occurring in a mammalian cell per day is high more than 60 000 per day Frequent occurrence of DNA damage is likely a problem for all DNA containing organisms and the need to cope with DNA damage and minimize their deleterious effects is likely a fundamental problem for life citation needed Most spontaneous mutations likely arise from error prone trans lesion synthesis past a DNA damage site in the template strand during DNA replication This process can overcome potentially lethal blockages but at the cost of introducing inaccuracies in daughter DNA The causal relationship of DNA damage to spontaneous mutation is illustrated by aerobically growing E coli bacteria in which 89 of spontaneously occurring base substitution mutations are caused by reactive oxygen species ROS induced DNA damage 26 In yeast more than 60 of spontaneous single base pair substitutions and deletions are likely caused by trans lesion synthesis 27 An additional significant source of mutations in eukaryotes is the inaccurate DNA repair process non homologous end joining that is often employed in repair of double strand breaks 28 In general it appears that the main underlying cause of spontaneous mutation is error prone trans lesion synthesis during DNA replication and that the error prone non homologous end joining repair pathway may also be an important contributor in eukaryotes Spontaneous hydrolysis edit DNA is not entirely stable in aqueous solution and depurination of the DNA can occur Under physiological conditions the glycosidic bond may be hydrolyzed spontaneously and 10 000 purine sites in DNA are estimated to be depurinated each day in a cell 20 Numerous DNA repair pathways exist for DNA however if the apurinic site is not repaired misincorporation of nucleotides may occur during replication Adenine is preferentially incorporated by DNA polymerases in an apurinic site Cytidine may also become deaminated to uridine at one five hundredth of the rate of depurination and can result in G to A transition Eukaryotic cells also contain 5 methylcytosine thought to be involved in the control of gene transcription which can become deaminated into thymine Tautomerism edit Main article Tautomer Tautomerization is the process by which compounds spontaneously rearrange themselves to assume their structural isomer forms For example the keto C O forms of guanine and thymine can rearrange into their rare enol OH forms while the amino NH2 forms of adenine and cytosine can result in the rarer imino NH forms In DNA replication tautomerization alters the base pairing sites and can cause the improper pairing of nucleic acid bases 29 Modification of bases edit Bases may be modified endogenously by normal cellular molecules For example DNA may be methylated by S adenosylmethionine thus altering the expression of the marked gene without incurring a mutation to the DNA sequence itself Histone modification is a related process in which the histone proteins around which DNA coils can be similarly modified via methylation phosphorylation or acetylation these modifications may act to alter gene expression of the local DNA and may also act to denote locations of damaged DNA in need of repair DNA may also be glycosylated by reducing sugars Many compounds such as PAHs aromatic amines aflatoxin and pyrrolizidine alkaloids may form reactive oxygen species catalyzed by cytochrome P450 These metabolites form adducts with the DNA which can cause errors in replication and the bulky aromatic adducts may form stable intercalation between bases and block replication The adducts may also induce conformational changes in the DNA Some adducts may also result in the depurination of the DNA 30 it is however uncertain how significant such depurination as caused by the adducts is in generating mutation Alkylation and arylation of bases can cause errors in replication Some alkylating agents such as N Nitrosamines may require the catalytic reaction of cytochrome P450 for the formation of a reactive alkyl cation N7 and O6 of guanine and the N3 and N7 of adenine are most susceptible to attack N7 guanine adducts form the bulk of DNA adducts but they appear to be non mutagenic Alkylation at O6 of guanine however is harmful because excision repair of O6 adduct of guanine may be poor in some tissues such as the brain 31 The O6 methylation of guanine can result in G to A transition while O4 methylthymine can be mispaired with guanine The type of the mutation generated however may be dependent on the size and type of the adduct as well as the DNA sequence 32 Ionizing radiation and reactive oxygen species often oxidize guanine to produce 8 oxoguanine See also Epigenetics nbsp Arrows indicates chromosomal breakages due to DNA damageBackbone damage edit Ionizing radiation may produce highly reactive free radicals that can break the bonds in the DNA Double stranded breakages are especially damaging and hard to repair producing translocation and deletion of part of a chromosome Alkylating agents like mustard gas may also cause breakages in the DNA backbone Oxidative stress may also generate highly reactive oxygen species that can damage DNA Incorrect repair of other damage induced by the highly reactive species can also lead to mutations Crosslinking edit Main article Crosslinking of DNA Covalent bonds between the bases of nucleotides in DNA be they in the same strand or opposing strands is referred to as crosslinking of DNA crosslinking of DNA may affect both the replication and the transcription of DNA and it may be caused by exposure to a variety of agents Some naturally occurring chemicals may also promote crosslinking such as psoralens after activation by UV radiation and nitrous acid Interstrand cross linking between two strands causes more damage as it blocks replication and transcription and can cause chromosomal breakages and rearrangements Some crosslinkers such as cyclophosphamide mitomycin C and cisplatin are used as anticancer chemotherapeutic because of their high degree of toxicity to proliferating cells Dimerization edit Main article Dimer Dimerization consists of the bonding of two monomers to form an oligomer such as the formation of pyrimidine dimers as a result of exposure to UV radiation which promotes the formation of a cyclobutyl ring between adjacent thymines in DNA 33 In human skin cells thousands of dimers may be formed in a day due to normal exposure to sunlight DNA polymerase h may help bypass these lesions in an error free manner 34 however individuals with defective DNA repair function such as those with xeroderma pigmentosum are sensitive to sunlight and may be prone to skin cancer nbsp Ethidium intercalated between two adenine thymine base pairs Clinically whether a tumor has formed as a direct consequence of UV radiation is discernible via DNA sequencing analysis for the characteristic context specific dimerization pattern that occurs due to excessive exposure to sunlight 35 Intercalation between bases edit Main article Intercalation biochemistry The planar structure of chemicals such as ethidium bromide and proflavine allows them to insert between bases in DNA This insert causes the DNA s backbone to stretch and makes slippage in DNA during replication more likely to occur since the bonding between the strands is made less stable by the stretching Forward slippage will result in deletion mutation while reverse slippage will result in an insertion mutation Also the intercalation into DNA of anthracyclines such as daunorubicin and doxorubicin interferes with the functioning of the enzyme topoisomerase II blocking replication as well as causing mitotic homologous recombination Insertional mutagenesis edit Main article Insertional mutagenesis Transposons and viruses or retrotransposons may insert DNA sequences into coding regions or functional elements of a gene and result in inactivation of the gene 36 Adaptive mutagenesis mechanisms edit Main article Adaptive mutation Adaptive mutagenesis has been defined as mutagenesis mechanisms that enable an organism to adapt to an environmental stress Since the variety of environmental stresses is very broad the mechanisms that enable it are also quite broad as far as research on the field has shown For instance in bacteria while modulation of the SOS response and endogenous prophage DNA synthesis has been shown to increase Acinetobacter baumannii resistance to ciprofloxacin 16 Resistance mechanisms are presumed to be linked to chromosomal mutation untransferable via horizontal gene transfer in some members of family Enterobacteriaceae such as E coli Salmonella spp Klebsiella spp and Enterobacter spp 37 Chromosomal events specially gene amplification seem also to be relevant to this adaptive mutagenesis in bacteria 38 Research in eukaryotic cells is much scarcer but chromosomal events seem also to be rather relevant while an ectopic intrachromosomal recombination has been reported to be involved in acquisition of resistance to 5 fluorocytosine in Saccharomyces cerevisiae 17 genome duplications have been found to confer resistance in S cerevisiae to nutrient poor environments 21 39 40 Laboratory applications editMain article Mutagenesis molecular biology technique In the laboratory mutagenesis is a technique by which DNA mutations are deliberately engineered to produce mutant genes proteins or strains of organisms Various constituents of a gene such as its control elements and its gene product may be mutated so that the function of a gene or protein can be examined in detail The mutation may also produce mutant proteins with altered properties or enhanced or novel functions that may prove to be of use commercially Mutant strains of organisms that have practical applications or allow the molecular basis of particular cell function to be investigated may also be produced Early methods of mutagenesis produced entirely random mutations however modern methods of mutagenesis are capable of producing site specific mutations Modern laboratory techniques used to generate these mutations include Directed mutagenesis Site directed mutagenesis PCR mutagenesis Insertional mutagenesis Signature tagged mutagenesis Transposon mutagenesis Sequence saturation mutagenesisSee also editCarcinogenesis DNA damage naturally occurring DNA repair Mutagen Mutation Mutation breeding Mutation rate TransfectionReferences edit Beale G 1993 The Discovery of Mustard Gas Mutagenesis by Auerbach and Robson in 1941 Genetics 134 2 393 399 doi 10 1093 genetics 134 2 393 PMC 1205483 PMID 8325476 Kevin M Gleason Published 2017 03 07 Hermann Joseph Muller s Study of X rays as a Mutagen 1926 1927 a href Template Cite web html title Template Cite web cite web a CS1 maint numeric names authors list link Genetics and Genomics Timeline 1927 Hermann J Muller 1890 1967 demonstrates that X rays can induce mutations Muller H J 1927 Artificial Transmutation of the Gene PDF Science 66 1699 84 87 Bibcode 1927Sci 66 84M doi 10 1126 science 66 1699 84 PMID 17802387 Crow J F Abrahamson S 1997 Seventy Years Ago Mutation Becomes Experimental Genetics 147 4 1491 1496 doi 10 1093 genetics 147 4 1491 PMC 1208325 PMID 9409815 Calabrese E J 30 June 2011 Muller s Nobel lecture on dose response for ionizing radiation ideology or science PDF Archives of Toxicology 85 4 1495 1498 doi 10 1007 s00204 011 0728 8 PMID 21717110 S2CID 4708210 Archived from the original PDF on 2 August 2017 Retrieved 30 December 2011 Ronald L Kathren December 2002 Historical Development of the Linear Nonthreshold Dose Response Model as Applied to Radiation University of New Hampshire Law Review 1 1 Stadler L J G F Sprague 1936 10 15 Genetic Effects of Ultra Violet Radiation in Maize I Unfiltered Radiation PDF Proc Natl Acad Sci U S A 22 10 572 8 Bibcode 1936PNAS 22 572S doi 10 1073 pnas 22 10 572 PMC 1076819 PMID 16588111 Retrieved 2007 10 11 Auerbach C Robson J M Carr J G March 1947 Chemical Production of Mutations Science 105 2723 243 7 Bibcode 1947Sci 105 243A doi 10 1126 science 105 2723 243 PMID 17769478 Brown J R Thornton J L 1957 Percivall Pott 1714 1788 and Chimney Sweepers Cancer of the Scrotum British Journal of Industrial Medicine 14 1 68 70 doi 10 1136 oem 14 1 68 PMC 1037746 PMID 13396156 Yamagawa K Ichikawa K 1915 Experimentelle Studie ueber die Pathogenese der Epithel geschwuelste Mitteilungen aus der Medizinischen Fakultat der Kaiserlichen Universitat zu Tokyo 15 295 344 Luch Andreas 2005 Nature and Nurture Lessons from Chemical Carcinogenesis Chemical Carcinogens From Past to Present Medscape Boyland E 1950 The biological significance of metabolism of polycyclic compounds Biochemical Society Symposium 5 40 54 ISSN 0067 8694 OCLC 216723160 Omura T Sato R 1962 A new cytochrome in liver microsomes The Journal of Biological Chemistry 237 4 1375 1376 doi 10 1016 S0021 9258 18 60338 2 PMID 14482007 Conney A H 1982 Induction of microsomal enzymes by foreign chemicals and carcinogenesis by polycyclic aromatic hydrocarbons G H A Clowes Memorial Lecture Cancer Research 42 12 4875 4917 PMID 6814745 a b Geisinger Edward Vargas Cuebas German Mortman Nadav J Syal Sapna Dai Yunfei Wainwright Elizabeth L Lazinski David Wood Stephen Zhu Zeyu 2019 06 11 Miller Samuel I ed The Landscape of Phenotypic and Transcriptional Responses to Ciprofloxacin in Acinetobacter baumannii Acquired Resistance Alleles Modulate Drug Induced SOS Response and Prophage Replication mBio 10 3 doi 10 1128 mBio 01127 19 ISSN 2150 7511 PMC 6561030 PMID 31186328 a b Quinto Alemany David Canerina Amaro Ana Hernandez Abad Luis G Machin Felix Romesberg Floyd E Gil Lamaignere Cristina 2012 07 31 Sturtevant Joy ed Yeasts Acquire Resistance Secondary to Antifungal Drug Treatment by Adaptive Mutagenesis PLOS ONE 7 7 e42279 Bibcode 2012PLoSO 742279Q doi 10 1371 journal pone 0042279 ISSN 1932 6203 PMC 3409178 PMID 22860105 Jha Alok 22 August 2012 Older fathers pass on more genetic mutations study shows The Guardian Kong A Frigge M L Masson G Besenbacher S Sulem P Magnusson G Gudjonsson S A Sigurdsson A Jonasdottir A Jonasdottir A Wong W S Sigurdsson G Walters G B Steinberg S Helgason H Thorleifsson G Gudbjartsson D F Helgason A Magnusson O T Thorsteinsdottir U Stefansson K 2012 Rate of de novo mutations and the importance of father s age to disease risk Nature 488 7412 471 475 Bibcode 2012Natur 488 471K doi 10 1038 nature11396 PMC 3548427 PMID 22914163 a b Loeb L A 1989 Endogenous carcinogenesis Molecular oncology into the twenty first century presidential address PDF Cancer Research 49 20 5489 5496 PMID 2676144 a b Heidenreich Erich January 2007 Adaptive Mutation in Saccharomyces cerevisiae Critical Reviews in Biochemistry and Molecular Biology 42 4 285 311 doi 10 1080 10409230701507773 ISSN 1040 9238 PMID 17687670 S2CID 11594730 Quinto Alemany David Canerina Amaro Ana Hernandez Abad Luis G Machin Felix Romesberg Floyd E Gil Lamaignere Cristina 2012 07 31 Sturtevant Joy ed Yeasts Acquire Resistance Secondary to Antifungal Drug Treatment by Adaptive Mutagenesis PLOS ONE 7 7 e42279 Bibcode 2012PLoSO 742279Q doi 10 1371 journal pone 0042279 ISSN 1932 6203 PMC 3409178 PMID 22860105 Aghapour Zahra Gholizadeh Pourya Ganbarov Khudaverdi bialvaei Abed Zahedi Mahmood Suhad Saad Tanomand Asghar Yousefi Mehdi Asgharzadeh Mohammad Yousefi Bahman April 2019 Molecular mechanisms related to colistin resistance in Enterobacteriaceae Infection and Drug Resistance 12 965 975 doi 10 2147 idr s199844 PMC 6519339 PMID 31190901 Trevor M Penning 2011 Chemical Carcinogenesis Current Cancer Research Springer ISBN 978 1617379949 Salnikow K Zhitkovich January 2008 Genetic and epigenetic mechanisms in metal carcinogenesis and cocarcinogenesis nickel arsenic and chromium Chemical Research in Toxicology 21 1 28 44 doi 10 1021 tx700198a PMC 2602826 PMID 17970581 Sakai A Nakanishi M Yoshiyama K Maki H July 2006 Impact of reactive oxygen species on spontaneous mutagenesis in Escherichia coli Genes Cells 11 7 767 78 doi 10 1111 j 1365 2443 2006 00982 x PMID 16824196 S2CID 1365658 Kunz BA Ramachandran K Vonarx EJ April 1998 DNA sequence analysis of spontaneous mutagenesis in Saccharomyces cerevisiae Genetics 148 4 1491 505 doi 10 1093 genetics 148 4 1491 PMC 1460101 PMID 9560369 Huertas P January 2010 DNA resection in eukaryotes deciding how to fix the break Nat Struct Mol Biol 17 1 11 6 doi 10 1038 nsmb 1710 PMC 2850169 PMID 20051983 Sinden Richard R 1994 DNA Structure and Function Academic Press pp 17 20 ISBN 978 0126457506 Melendez Colon V J Smith C A Seidel A Luch A Platt K L Baird W M 1997 Formation of stable adducts and absence of depurinating DNA adducts in cells and DNA treated with the potent carcinogen dibenzoa lpyrene or its diol epoxides Proceedings of the National Academy of Sciences of the United States of America 94 25 13542 13547 Bibcode 1997PNAS 9413542M doi 10 1073 pnas 94 25 13542 PMC 28342 PMID 9391062 Boysen G Pachkowski B F Nakamura J Swenberg J A 2009 The Formation and Biological Significance of N7 Guanine Adducts Mutation Research Genetic Toxicology and Environmental Mutagenesis 678 2 76 94 doi 10 1016 j mrgentox 2009 05 006 PMC 2739241 PMID 19465146 Loechler E L 1996 The role of adduct site specific mutagenesis in understanding how carcinogen DNA adducts cause mutations Perspective prospects and problems Carcinogenesis 17 5 895 902 doi 10 1093 carcin 17 5 895 PMID 8640935 Setlow R B 1966 Cyclobutane type pyrimidine dimers in polynucleotides Science 153 734 379 386 Bibcode 1966Sci 153 379S doi 10 1126 science 153 3734 379 PMID 5328566 S2CID 11210761 Broyde S Patel D J 2010 DNA repair How to accurately bypass damage Nature 465 7301 1023 1024 Bibcode 2010Natur 465 1023B doi 10 1038 4651023a PMC 4986998 PMID 20577203 Mata Douglas A Williams Erik A Sokol Ethan Oxnard Geoffrey R Fleischmann Zoe Tse Julie Y Decker Brennan 23 March 2022 Prevalence of UV Mutational Signatures Among Cutaneous Primary Tumors JAMA Network Open 5 3 e223833 doi 10 1001 jamanetworkopen 2022 3833 PMC 8943639 PMID 35319765 Mohanasundaram Boominathan Rajmane Vyankatesh B Jogdand Sukanya V Bhide Amey J Banerjee Anjan K June 2019 Agrobacterium mediated Tnt1 mutagenesis of moss protonemal filaments and generation of stable mutants with impaired gametophyte Molecular Genetics and Genomics 294 3 583 596 doi 10 1007 s00438 019 01532 4 PMID 30689096 S2CID 59304089 Aghapour Zahra Gholizadeh Pourya Ganbarov Khudaverdi bialvaei Abed Zahedi Mahmood Suhad Saad Tanomand Asghar Yousefi Mehdi Asgharzadeh Mohammad Yousefi Bahman April 2019 Molecular mechanisms related to colistin resistance in Enterobacteriaceae Infection and Drug Resistance 12 965 975 doi 10 2147 idr s199844 PMC 6519339 PMID 31190901 Hersh Megan N Ponder Rebecca G Hastings P J Rosenberg Susan M June 2004 Adaptive mutation and amplification in Escherichia coli two pathways of genome adaptation under stress Research in Microbiology 155 5 352 359 doi 10 1016 j resmic 2004 01 020 PMID 15207867 Longerich S Galloway A M Harris R S Wong C Rosenberg S M 1995 12 19 Adaptive mutation sequences reproduced by mismatch repair deficiency Proceedings of the National Academy of Sciences 92 26 12017 12020 Bibcode 1995PNAS 9212017L doi 10 1073 pnas 92 26 12017 ISSN 0027 8424 PMC 40287 PMID 8618835 Rosenberg Susan M Fitzgerald Devon M 2019 04 01 What is mutation A chapter in the series How microbes jeopardize the modern synthesis PLOS Genetics 15 4 e1007995 doi 10 1371 journal pgen 1007995 ISSN 1553 7404 PMC 6443146 PMID 30933985 nbsp Look up mutagenesis in Wiktionary the free dictionary Retrieved from https en wikipedia org w index php title Mutagenesis amp oldid 1195978504, wikipedia, wiki, book, books, library,

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