fbpx
Wikipedia

Splice site mutation

November 28, 2023

A splice site mutation is a genetic mutation that inserts, deletes or changes a number of nucleotides in the specific site at which splicing takes place during the processing of precursor messenger RNA into mature messenger RNA. Splice site consensus sequences that drive exon recognition are located at the very termini of introns.[1] The deletion of the splicing site results in one or more introns remaining in mature mRNA and may lead to the production of abnormal proteins. When a splice site mutation occurs, the mRNA transcript possesses information from these introns that normally should not be included. Introns are supposed to be removed, while the exons are expressed.

The mutation must occur at the specific site at which intron splicing occurs: within non-coding sites in a gene, directly next to the location of the exon. The mutation can be an insertion, deletion, frameshift, etc. The splicing process itself is controlled by the given sequences, known as splice-donor and splice-acceptor sequences, which surround each exon. Mutations in these sequences may lead to retention of large segments of intronic DNA by the mRNA, or to entire exons being spliced out of the mRNA. These changes could result in production of a nonfunctional protein.[2] An intron is separated from its exon by means of the splice site. Acceptor-site and donor-site relating to the splice sites signal to the spliceosome where the actual cut should be made. These donor sites, or recognition sites, are essential in the processing of mRNA. The average vertebrate gene consists of multiple small exons (average size, 137 nucleotides) separated by introns that are considerably larger.[1]

A visual representation of a splice site mutation instance[3]

Background edit

In 1993, Richard J. Roberts and Phillip Allen Sharp received the Nobel Prize in Physiology or Medicine for their discovery of "split genes".[4] Using the model adenovirus in their research, they were able to discover splicing—the fact that pre-mRNA is processed into mRNA once introns were removed from the RNA segment. These two scientists discovered the existence of splice sites, thereby changing the face of genomics research. They also discovered that the splicing of the messenger RNA can occur in different ways, opening up the possibility for a mutation to occur.

Technology edit

Today, many different types of technologies exist in which splice sites can be located and analyzed for more information. The Human Splicing Finder is an online database stemming from the Human Genome Project data. The genome database identifies thousands of mutations related to medical and health fields, as well as providing critical research information regarding splice site mutations. The tool specifically searches for pre-mRNA splicing errors, the calculation of potential splice sites using complex algorithms, and correlation with several other online genomic databases, such as the Ensembl genome browser.[5]

Role in Disease edit

Due to the sensitive location of splice sites, mutations in the acceptor or donor areas of splice sites can become detrimental to a human individual. In fact, many different types of diseases stem from anomalies within the splice sites.

Cancer edit

A study researching the role of splice site mutations in cancer supported that a splice site mutation was common in a set of women who were positive for breast and ovarian cancer. These women had the same mutation, according to the findings. An intronic single base-pair substitution destroys an acceptor site, thus activating a cryptic splice site, leading to a 59 base-pair insertion and chain termination. The four families with both breast and ovarian cancer had chain termination mutations in the N-terminal half of the protein.[6] The mutation in this research example was located within the splice-site.

Dementia edit

According to a research study conducted Hutton, M et al, a missense mutation occurring on the 5' region of the RNA associated with the tau protein was found to be correlated with inherited dementia (known as FTDP-17). The splice-site mutations all destabilize a potential stem–loop structure which is most likely involved in regulating the alternative splicing of exon10 in chromosome 17. Consequently, more usage occurs on the 5' splice site and an increased proportion of tau transcripts that include exon 10 are created. Such drastic increase in mRNA will increase the proportion of Tau containing four microtubule-binding repeats, which is consistent with the neuropathology described in several families with FTDP-17, a type inherited dementia.[7]

Epilepsy edit

Some types of epilepsy may be brought on due to a splice site mutation. In addition to a mutation in a stop codon, a splice site mutation on the 3' strand was found in a gene coding for cystatin B in Progressive Myoclonus Epilepsy[8] patients. This combination of mutations was not found in unaffected individuals. By comparing sequences with and without the splice site mutation, investigators were able to determine that a G-to-C nucleotide transversion occurs at the last position of the first intron. This transversion occurs in the region that codes for the cystatin B gene. Individuals suffering from Progressive Myoclonus Epilepsy possess a mutated form of this gene, which results in decreased output of mature mRNA, and subsequently decreases in protein expression.

A study has also shown that a type of Childhood Absence Epilepsy (CAE) causing febrile seizures may be linked to a splice site mutation in the sixth intron of the GABRG2 gene. This splice site mutation was found to cause a nonfunctional GABRG2 subunit in affected individuals.[9] According to this study, a point mutation was the culprit for the splice-donor site mutation, which occurred in intron 6. A nonfunctional protein product is produced, leading to the also nonfunctional subunit.

Hematological Disorders edit

Several genetic diseases may be the result of splice site mutations. For example, mutations that cause the incorrect splicing of β-globin mRNA are responsible of some cases of β-thalassemia. Another Example is TTP (thrombotic thrombocytopenic purpura). TTP is caused by deficiency of ADAMTS-13. A splice site mutation of ADAMTS-13 gene can therefore cause TTP. It is estimated that 15% of all point mutations causing human genetic diseases occur within a splice site.[10]

Parathyroid Deficiency edit

When a splice site mutation occurs in intron 2 of the gene that produces the parathyroid hormone, a parathyroid deficiency can prevail. In one particular study, a G to C substitution in the splice site of intron 2 produces a skipping effect in the messenger RNA transcript. The exon that is skipped possesses the initiation start codon to produce parathyroid hormone.[11] Such failure in initiation causes the deficiency.

Analysis edit

Using the model organism Drosophila melanogaster, data has been compiled regarding the genomic information and sequencing of this organism. A prediction model exists in which a researcher can upload his or her genomic information and use a splice site prediction database to gather information about where the splice sites could be located. The Berkeley Drosophila Project can be used to incorporate this research, as well as annotate high quality euchromatic data. The splice site predictor can be a great tool for researchers studying human disease in this model organism.

Splice site mutations can be analyzed using information theory.[12]

References edit

  1. ^ a b Berget, Susan (1995). "Exon Recognition in Vertebrate Splicing". The Journal of Biological Chemistry. 270 (6): 2411–2414. doi:10.1074/jbc.270.6.2411. PMID 7852296.
  2. ^ Understanding Cancer Genomics: Splice Site Mutations. National Cancer Institute.
  3. ^ Understanding Cancer Genomics. National Cancer Institute.
  4. ^ "Physiology or Medicine 1993 - Press Release". www.nobelprize.org. Retrieved 2017-10-07.
  5. ^ "The Human Splicing Finder".
  6. ^ Friedman, Lori (1994). "Confirmation of BRCA1 by analysis of germline mutations linked to breast and ovarian cancer in ten families". Nature Genetics. 8 (4): 399–404. doi:10.1038/ng1294-399. PMID 7894493. S2CID 2863113.
  7. ^ Hutton, Mike; Lendon, Corinne; Rizzu, Patrizia; Baker, Matt (18 June 1998). "Association of missense and 5'-splice-site mutations in tau with the inherited dementia FTDP-17". Nature. 393 (6686): 702–705. Bibcode:1998Natur.393..702H. doi:10.1038/31508. PMID 9641683. S2CID 205001265.
  8. ^ Pennacchio, Len A.; Lehesjoki, Anna-Elina; Stone, Nancy E.; Wilour, Virginia L. (Mar 22, 1996). "Mutations in the Gene Encoding Cystatin B in Progressive Myoclonus Epilepsy (EPM1)". Science. 271 (5256): 1731–1734. Bibcode:1996Sci...271.1731P. doi:10.1126/science.271.5256.1731. JSTOR 2890839. PMID 8596935. S2CID 84361089.
  9. ^ Kananura, Colette; Haug, Karsten; Sander, Thomas; Runge, Uwe; Gu, Wenli; Hallmann, Kerstin; Rebstock, Johannes; Heils, Armin; Steinlein, Ortrud (July 2002). "A Splice-Site Mutation in GABRG2 Associated With Childhood Absence Epilepsy and Febrile Convulsions". Arch Neurol. 59 (7): 1137–1141. doi:10.1001/archneur.59.7.1137. PMID 12117362.
  10. ^ Carvalho, Gisah A; Weiss, Roy E; Refetoff, Samuel (June 22, 1998). "Complete Thyroxine-Binding Globulin (TBG) Deficiency Produced by a Mutation in Acceptor Splice Site Causing Frameshift and Early Termination of Translation (TBG-Kankakee)". The Journal of Clinical Endocrinology and Metabolism. 83 (10): 3604–3608. doi:10.1210/jcem.83.10.5208. PMID 9768672.
  11. ^ Parkinson, David B.; Thakker, Rajesh V. (1992). "A donor splice site mutation in the parathyroid hormone gene is associated with autosomal recessive hypoparathyroidism". Nature Genetics. 1 (2): 149–152. doi:10.1038/ng0592-149. PMID 1302009. S2CID 24032313.
  12. ^ Rogan, PK; Faux, BM; Schneider, TD (1998). "Information analysis of human splice site mutations". Hum. Mutat. 12 (3): 153–71. doi:10.1002/(SICI)1098-1004(1998)12:3<153::AID-HUMU3>3.0.CO;2-I. PMID 9711873.

November 28, 2023
splice, site, mutation, splice, site, mutation, genetic, mutation, that, inserts, deletes, changes, number, nucleotides, specific, site, which, splicing, takes, place, during, processing, precursor, messenger, into, mature, messenger, splice, site, consensus, . A splice site mutation is a genetic mutation that inserts deletes or changes a number of nucleotides in the specific site at which splicing takes place during the processing of precursor messenger RNA into mature messenger RNA Splice site consensus sequences that drive exon recognition are located at the very termini of introns 1 The deletion of the splicing site results in one or more introns remaining in mature mRNA and may lead to the production of abnormal proteins When a splice site mutation occurs the mRNA transcript possesses information from these introns that normally should not be included Introns are supposed to be removed while the exons are expressed The mutation must occur at the specific site at which intron splicing occurs within non coding sites in a gene directly next to the location of the exon The mutation can be an insertion deletion frameshift etc The splicing process itself is controlled by the given sequences known as splice donor and splice acceptor sequences which surround each exon Mutations in these sequences may lead to retention of large segments of intronic DNA by the mRNA or to entire exons being spliced out of the mRNA These changes could result in production of a nonfunctional protein 2 An intron is separated from its exon by means of the splice site Acceptor site and donor site relating to the splice sites signal to the spliceosome where the actual cut should be made These donor sites or recognition sites are essential in the processing of mRNA The average vertebrate gene consists of multiple small exons average size 137 nucleotides separated by introns that are considerably larger 1 A visual representation of a splice site mutation instance 3 Contents 1 Background 2 Technology 3 Role in Disease 3 1 Cancer 3 2 Dementia 3 3 Epilepsy 3 4 Hematological Disorders 3 5 Parathyroid Deficiency 4 Analysis 5 ReferencesBackground editIn 1993 Richard J Roberts and Phillip Allen Sharp received the Nobel Prize in Physiology or Medicine for their discovery of split genes 4 Using the model adenovirus in their research they were able to discover splicing the fact that pre mRNA is processed into mRNA once introns were removed from the RNA segment These two scientists discovered the existence of splice sites thereby changing the face of genomics research They also discovered that the splicing of the messenger RNA can occur in different ways opening up the possibility for a mutation to occur Technology editToday many different types of technologies exist in which splice sites can be located and analyzed for more information The Human Splicing Finder is an online database stemming from the Human Genome Project data The genome database identifies thousands of mutations related to medical and health fields as well as providing critical research information regarding splice site mutations The tool specifically searches for pre mRNA splicing errors the calculation of potential splice sites using complex algorithms and correlation with several other online genomic databases such as the Ensembl genome browser 5 Role in Disease editDue to the sensitive location of splice sites mutations in the acceptor or donor areas of splice sites can become detrimental to a human individual In fact many different types of diseases stem from anomalies within the splice sites Cancer edit A study researching the role of splice site mutations in cancer supported that a splice site mutation was common in a set of women who were positive for breast and ovarian cancer These women had the same mutation according to the findings An intronic single base pair substitution destroys an acceptor site thus activating a cryptic splice site leading to a 59 base pair insertion and chain termination The four families with both breast and ovarian cancer had chain termination mutations in the N terminal half of the protein 6 The mutation in this research example was located within the splice site Dementia edit According to a research study conducted Hutton M et al a missense mutation occurring on the 5 region of the RNA associated with the tau protein was found to be correlated with inherited dementia known as FTDP 17 The splice site mutations all destabilize a potential stem loop structure which is most likely involved in regulating the alternative splicing of exon10 in chromosome 17 Consequently more usage occurs on the 5 splice site and an increased proportion of tau transcripts that include exon 10 are created Such drastic increase in mRNA will increase the proportion of Tau containing four microtubule binding repeats which is consistent with the neuropathology described in several families with FTDP 17 a type inherited dementia 7 Epilepsy edit Some types of epilepsy may be brought on due to a splice site mutation In addition to a mutation in a stop codon a splice site mutation on the 3 strand was found in a gene coding for cystatin B in Progressive Myoclonus Epilepsy 8 patients This combination of mutations was not found in unaffected individuals By comparing sequences with and without the splice site mutation investigators were able to determine that a G to C nucleotide transversion occurs at the last position of the first intron This transversion occurs in the region that codes for the cystatin B gene Individuals suffering from Progressive Myoclonus Epilepsy possess a mutated form of this gene which results in decreased output of mature mRNA and subsequently decreases in protein expression A study has also shown that a type of Childhood Absence Epilepsy CAE causing febrile seizures may be linked to a splice site mutation in the sixth intron of the GABRG2 gene This splice site mutation was found to cause a nonfunctional GABRG2 subunit in affected individuals 9 According to this study a point mutation was the culprit for the splice donor site mutation which occurred in intron 6 A nonfunctional protein product is produced leading to the also nonfunctional subunit Hematological Disorders edit Several genetic diseases may be the result of splice site mutations For example mutations that cause the incorrect splicing of b globin mRNA are responsible of some cases of b thalassemia Another Example is TTP thrombotic thrombocytopenic purpura TTP is caused by deficiency of ADAMTS 13 A splice site mutation of ADAMTS 13 gene can therefore cause TTP It is estimated that 15 of all point mutations causing human genetic diseases occur within a splice site 10 Parathyroid Deficiency edit When a splice site mutation occurs in intron 2 of the gene that produces the parathyroid hormone a parathyroid deficiency can prevail In one particular study a G to C substitution in the splice site of intron 2 produces a skipping effect in the messenger RNA transcript The exon that is skipped possesses the initiation start codon to produce parathyroid hormone 11 Such failure in initiation causes the deficiency Analysis editUsing the model organism Drosophila melanogaster data has been compiled regarding the genomic information and sequencing of this organism A prediction model exists in which a researcher can upload his or her genomic information and use a splice site prediction database to gather information about where the splice sites could be located The Berkeley Drosophila Project can be used to incorporate this research as well as annotate high quality euchromatic data The splice site predictor can be a great tool for researchers studying human disease in this model organism Splice site mutations can be analyzed using information theory 12 References edit a b Berget Susan 1995 Exon Recognition in Vertebrate Splicing The Journal of Biological Chemistry 270 6 2411 2414 doi 10 1074 jbc 270 6 2411 PMID 7852296 Understanding Cancer Genomics Splice Site Mutations National Cancer Institute Understanding Cancer Genomics National Cancer Institute Physiology or Medicine 1993 Press Release www nobelprize org Retrieved 2017 10 07 The Human Splicing Finder Friedman Lori 1994 Confirmation of BRCA1 by analysis of germline mutations linked to breast and ovarian cancer in ten families Nature Genetics 8 4 399 404 doi 10 1038 ng1294 399 PMID 7894493 S2CID 2863113 Hutton Mike Lendon Corinne Rizzu Patrizia Baker Matt 18 June 1998 Association of missense and 5 splice site mutations in tau with the inherited dementia FTDP 17 Nature 393 6686 702 705 Bibcode 1998Natur 393 702H doi 10 1038 31508 PMID 9641683 S2CID 205001265 Pennacchio Len A Lehesjoki Anna Elina Stone Nancy E Wilour Virginia L Mar 22 1996 Mutations in the Gene Encoding Cystatin B in Progressive Myoclonus Epilepsy EPM1 Science 271 5256 1731 1734 Bibcode 1996Sci 271 1731P doi 10 1126 science 271 5256 1731 JSTOR 2890839 PMID 8596935 S2CID 84361089 Kananura Colette Haug Karsten Sander Thomas Runge Uwe Gu Wenli Hallmann Kerstin Rebstock Johannes Heils Armin Steinlein Ortrud July 2002 A Splice Site Mutation in GABRG2 Associated With Childhood Absence Epilepsy and Febrile Convulsions Arch Neurol 59 7 1137 1141 doi 10 1001 archneur 59 7 1137 PMID 12117362 Carvalho Gisah A Weiss Roy E Refetoff Samuel June 22 1998 Complete Thyroxine Binding Globulin TBG Deficiency Produced by a Mutation in Acceptor Splice Site Causing Frameshift and Early Termination of Translation TBG Kankakee The Journal of Clinical Endocrinology and Metabolism 83 10 3604 3608 doi 10 1210 jcem 83 10 5208 PMID 9768672 Parkinson David B Thakker Rajesh V 1992 A donor splice site mutation in the parathyroid hormone gene is associated with autosomal recessive hypoparathyroidism Nature Genetics 1 2 149 152 doi 10 1038 ng0592 149 PMID 1302009 S2CID 24032313 Rogan PK Faux BM Schneider TD 1998 Information analysis of human splice site mutations Hum Mutat 12 3 153 71 doi 10 1002 SICI 1098 1004 1998 12 3 lt 153 AID HUMU3 gt 3 0 CO 2 I PMID 9711873 Retrieved from https en wikipedia org w index php title Splice site mutation amp oldid 1170993574, wikipedia, wiki, book, books, library,

article

, read, download, free, free download, mp3, video, mp4, 3gp, jpg, jpeg, gif, png, picture, music, song, movie, book, game, games.