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Literature DB >> 22926731

Cancer-associated variants and a common polymorphism of MUTYH exhibit reduced repair of oxidative DNA damage using a GFP-based assay in mammalian cells.

Alan G Raetz¹, Yali Xie, Sucharita Kundu, Megan K Brinkmeyer, Cindy Chang, Sheila S David.

Abstract

Biallelic germline mutations in the base excision repair enzyme gene MUTYH lead to multiple colorectal adenomas and carcinomas referred to as MUTYH-associated polyposis. MUTYH removes adenine misincorporated opposite the DNA oxidation product, 8-oxoguanine (OG), thereby preventing accumulation of G:C to T:A transversion mutations. The most common cancer-associated MUTYH variant proteins when expressed in bacteria exhibit reduced OG:A mismatch affinity and adenine removal activity. However, direct evaluation of OG:A mismatch repair efficiency in mammalian cells has not been assessed due to the lack of an appropriate assay. To address this, we developed a novel fluorescence-based assay of OG:A repair and measured the repair capacity of MUTYH-associated polyposis variants expressed in Mutyh-/- mouse embryonic fibroblasts (MEFs). The repair of a single site-specific synthetic lesion in a green fluorescent protein reporter leads to green fluorescent protein expression with co-expression of a red fluorescent protein serving as the transfection control. Cell lines that stably express the MUTYH-associated polyposis variants G382D and Y165C have significantly lower OG:A repair versus wild-type MEFs and MEFs expressing human wild-type MUTYH. The MUTYH allele that encodes the Q324H variant is found at a frequency above 40% in samples from different ethnic groups and has long been considered phenotypically silent but has recently been associated with increased cancer risk in several clinical studies. In vitro analysis of Q324H MUTYH expressed in insect cells showed that it has reduced enzyme activity similar to that of the known cancer variant G382D. Moreover, we find that OG:A repair in MEFs expressing Q324H was significantly lower than wild-type controls, establishing that Q324H is functionally impaired and providing further evidence that this common variant may lead to increased cancer risk.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：

Year: 2012 PMID： 22926731 PMCID： PMC3483017 DOI： 10.1093/carcin/bgs270

Source DB: PubMed Journal: Carcinogenesis ISSN： 0143-3334 Impact factor: 4.944

52 in total

1. Human homolog of the MutY repair protein (hMYH) physically interacts with proteins involved in long patch DNA base excision repair.

Authors: A Parker; Y Gu; W Mahoney; S H Lee; K K Singh; A L Lu
Journal: J Biol Chem Date: 2000-11-22 Impact factor: 5.157

2. Inherited defects in the DNA glycosylase MYH cause multiple colorectal adenoma and carcinoma.

Authors: Jeremy P Cheadle; Sunil Dolwani; Julian R Sampson
Journal: Carcinogenesis Date: 2003-05-09 Impact factor: 4.944

3. Human MutY homolog, a DNA glycosylase involved in base excision repair, physically and functionally interacts with mismatch repair proteins human MutS homolog 2/human MutS homolog 6.

Authors: Yesong Gu; Antony Parker; Teresa M Wilson; Haibo Bai; Dau-Yin Chang; A-Lien Lu
Journal: J Biol Chem Date: 2002-01-18 Impact factor: 5.157

4. Insight into the functional consequences of inherited variants of the hMYH adenine glycosylase associated with colorectal cancer: complementation assays with hMYH variants and pre-steady-state kinetics of the corresponding mutated E.coli enzymes.

Authors: Nikolas H Chmiel; Alison L Livingston; Sheila S David
Journal: J Mol Biol Date: 2003-03-21 Impact factor: 5.469

5. Inherited variants of MYH associated with somatic G:C-->T:A mutations in colorectal tumors.

Authors: Nada Al-Tassan; Nikolas H Chmiel; Julie Maynard; Nick Fleming; Alison L Livingston; Geraint T Williams; Angela K Hodges; D Rhodri Davies; Sheila S David; Julian R Sampson; Jeremy P Cheadle
Journal: Nat Genet Date: 2002-01-30 Impact factor: 38.330

6. Multiple colorectal adenomas, classic adenomatous polyposis, and germ-line mutations in MYH.

Authors: Oliver M Sieber; Lara Lipton; Michael Crabtree; Karl Heinimann; Paulo Fidalgo; Robin K S Phillips; Marie-Luise Bisgaard; Torben F Orntoft; Lauri A Aaltonen; Shirley V Hodgson; Huw J W Thomas; Ian P M Tomlinson
Journal: N Engl J Med Date: 2003-02-27 Impact factor: 91.245

7. Carcinogenesis in MYH-associated polyposis follows a distinct genetic pathway.

Authors: Lara Lipton; Sarah E Halford; Victoria Johnson; Marco R Novelli; Angela Jones; Carole Cummings; Ella Barclay; Oliver Sieber; Amir Sadat; Marie-Luise Bisgaard; Shirley V Hodgson; Lauri A Aaltonen; Huw J W Thomas; Ian P M Tomlinson
Journal: Cancer Res Date: 2003-11-15 Impact factor: 12.701

8. Comprehensive analysis of the contribution of germline MYH variation to early-onset colorectal cancer.

Authors: Christina Fleischmann; Julian Peto; Jeremy Cheadle; Bindiya Shah; Julian Sampson; Richard S Houlston
Journal: Int J Cancer Date: 2004-04-20 Impact factor: 7.396

9. Structural basis for removal of adenine mispaired with 8-oxoguanine by MutY adenine DNA glycosylase.

Authors: J Christopher Fromme; Anirban Banerjee; Susan J Huang; Gregory L Verdine
Journal: Nature Date: 2004-02-12 Impact factor: 49.962

10. The mammalian mismatch repair pathway removes DNA 8-oxodGMP incorporated from the oxidized dNTP pool.

Authors: Claudia Colussi; Eleonora Parlanti; Paolo Degan; Gabriele Aquilina; Deborah Barnes; Peter Macpherson; Peter Karran; Marco Crescenzi; Eugenia Dogliotti; Margherita Bignami
Journal: Curr Biol Date: 2002-06-04 Impact factor: 10.834

23 in total

1. Distinct functional consequences of MUTYH variants associated with colorectal cancer: Damaged DNA affinity, glycosylase activity and interaction with PCNA and Hus1.

Authors: Megan K Brinkmeyer; Sheila S David
Journal: DNA Repair (Amst) Date: 2015-08-12

Review 2. Repair of 8-oxoG:A mismatches by the MUTYH glycosylase: Mechanism, metals and medicine.

Authors: Douglas M Banda; Nicole N Nuñez; Michael A Burnside; Katie M Bradshaw; Sheila S David
Journal: Free Radic Biol Med Date: 2017-01-10 Impact factor: 7.376

3. Inter-individual variation in DNA repair capacity: a need for multi-pathway functional assays to promote translational DNA repair research.

Authors: Zachary D Nagel; Isaac A Chaim; Leona D Samson
Journal: DNA Repair (Amst) Date: 2014-04-26

4. Increased risk for colorectal adenomas and cancer in mono-allelic MUTYH mutation carriers: results from a cohort of North-African Jews.

Authors: Guy Rosner; Dani Bercovich; Yael Etzion Daniel; Hana Strul; Naomi Fliss-Isakov; Meirav Ben-Yehoiada; Erwin Santo; Zamir Halpern; Revital Kariv
Journal: Fam Cancer Date: 2015-09 Impact factor: 2.375

Review 10. Functional interplay between ATM/ATR-mediated DNA damage response and DNA repair pathways in oxidative stress.

Authors: Shan Yan; Melanie Sorrell; Zachary Berman
Journal: Cell Mol Life Sci Date: 2014-06-20 Impact factor: 9.261