Literature DB >> 19836313

Adenine removal activity and bacterial complementation with the human MutY homologue (MUTYH) and Y165C, G382D, P391L and Q324R variants associated with colorectal cancer.

Sucharita Kundu1, Megan K Brinkmeyer, Alison L Livingston, Sheila S David.   

Abstract

MUTYH-associated polyposis (MAP) is the only inherited colorectal cancer syndrome that is associated with inherited biallelic mutations in a base excision repair gene. The MUTYH glycosylase plays an important role in preventing mutations associated with 8-oxoguanine (OG) by removing adenine residues that have been misincorporated opposite OG. MAP-associated mutations are present throughout MUTYH, with a large number coding for missense variations. To date the available information on the functional properties of MUTYH variants is conflicting. In this study, a kinetic analysis of the adenine glycosylase activity of MUTYH and several variants was undertaken using a correction for active fraction to control for differences due to overexpression and purification. Using these methods, the rate constants for steps involved in the adenine removal process were determined for the MAP variants Y165C, G382D, P391L and Q324R MUTYH. Under single-turnover conditions, the rate of adenine removal for these four variants was found to be 30-40% of WT MUTYH. In addition, the ability of MUTYH and the variants to suppress mutations and complement for the absence of MutY in Escherichia coli was assessed using rifampicin resistance assays. The presence of WT and Q324R MUTYH resulted in complete suppression of the mutation frequency, while G382D MUTYH showed reduced ability to suppress the mutation frequency. In contrast, the mutation frequency observed upon expression of P391L and Y165C MUTYH were similar to the controls, suggesting no activity toward preventing DNA mutations. Notably, though all variations studied herein resulted in similar reductions in adenine glycosylase activity, the effects in the bacterial complementation are quite different. This suggests that the consequences of a specific amino acid variation on overall repair in a cellular context may be magnified.

Entities:  

Mesh:

Substances:

Year:  2009        PMID: 19836313      PMCID: PMC2789978          DOI: 10.1016/j.dnarep.2009.09.009

Source DB:  PubMed          Journal:  DNA Repair (Amst)        ISSN: 1568-7856


  52 in total

1.  A single engineered point mutation in the adenine glycosylase MutY confers bifunctional glycosylase/AP lyase activity.

Authors:  S D Williams; S S David
Journal:  Biochemistry       Date:  2000-08-22       Impact factor: 3.162

Review 2.  Mechanisms of formation, genotoxicity, and mutation of guanine oxidation products.

Authors:  William L Neeley; John M Essigmann
Journal:  Chem Res Toxicol       Date:  2006-04       Impact factor: 3.739

Review 3.  The intricate structural chemistry of base excision repair machinery: implications for DNA damage recognition, removal, and repair.

Authors:  Kenichi Hitomi; Shigenori Iwai; John A Tainer
Journal:  DNA Repair (Amst)       Date:  2007-01-08

Review 4.  Roles of base excision repair subpathways in correcting oxidized abasic sites in DNA.

Authors:  Jung-Suk Sung; Bruce Demple
Journal:  FEBS J       Date:  2006-04       Impact factor: 5.542

Review 5.  Base-excision repair of oxidative DNA damage.

Authors:  Sheila S David; Valerie L O'Shea; Sucharita Kundu
Journal:  Nature       Date:  2007-06-21       Impact factor: 49.962

6.  Site-directed mutagenesis of the cysteine ligands to the [4Fe-4S] cluster of Escherichia coli MutY.

Authors:  M P Golinelli; N H Chmiel; S S David
Journal:  Biochemistry       Date:  1999-06-01       Impact factor: 3.162

7.  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

8.  Autosomal recessive colorectal adenomatous polyposis due to inherited mutations of MYH.

Authors:  Julian R Sampson; Sunil Dolwani; Sian Jones; Diana Eccles; Anthony Ellis; D Gareth Evans; Ian Frayling; Sheila Jordan; Eamonn R Maher; Tony Mak; Julie Maynard; Francesca Pigatto; Joan Shaw; Jeremy P Cheadle
Journal:  Lancet       Date:  2003-07-05       Impact factor: 79.321

9.  Evidence that MutY is a monofunctional glycosylase capable of forming a covalent Schiff base intermediate with substrate DNA.

Authors:  S D Williams; S S David
Journal:  Nucleic Acids Res       Date:  1998-11-15       Impact factor: 16.971

10.  Characterization of mutant MUTYH proteins associated with familial colorectal cancer.

Authors:  Mohsin Ali; Hyeja Kim; Sean Cleary; Claire Cupples; Steven Gallinger; Robert Bristow
Journal:  Gastroenterology       Date:  2008-05-07       Impact factor: 22.682
View more
  26 in total

1.  Ser 524 is a phosphorylation site in MUTYH and Ser 524 mutations alter 8-oxoguanine (OG): a mismatch recognition.

Authors:  Sucharita Kundu; Megan K Brinkmeyer; Richard A Eigenheer; Sheila S David
Journal:  DNA Repair (Amst)       Date:  2010-08-17

2.  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 3.  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

4.  Steady-state, pre-steady-state, and single-turnover kinetic measurement for DNA glycosylase activity.

Authors:  Akira Sassa; William A Beard; David D Shock; Samuel H Wilson
Journal:  J Vis Exp       Date:  2013-08-19       Impact factor: 1.355

5.  Catalytic contributions of key residues in the adenine glycosylase MutY revealed by pH-dependent kinetics and cellular repair assays.

Authors:  Megan K Brinkmeyer; Mary Ann Pope; Sheila S David
Journal:  Chem Biol       Date:  2012-02-24

6.  The DNA repair enzyme MUTYH potentiates cytotoxicity of the alkylating agent MNNG by interacting with abasic sites.

Authors:  Alan G Raetz; Douglas M Banda; Xiaoyan Ma; Gege Xu; Anisha N Rajavel; Paige L McKibbin; Carlito B Lebrilla; Sheila S David
Journal:  J Biol Chem       Date:  2020-01-30       Impact factor: 5.157

Review 7.  When you're strange: Unusual features of the MUTYH glycosylase and implications in cancer.

Authors:  Alan G Raetz; Sheila S David
Journal:  DNA Repair (Amst)       Date:  2019-06-08

8.  A structural hinge in eukaryotic MutY homologues mediates catalytic activity and Rad9-Rad1-Hus1 checkpoint complex interactions.

Authors:  Paz J Luncsford; Dau-Yin Chang; Guoli Shi; Jade Bernstein; Amrita Madabushi; Dimeka N Patterson; A-Lien Lu; Eric A Toth
Journal:  J Mol Biol       Date:  2010-09-15       Impact factor: 5.469

9.  Mutants of the base excision repair glycosylase, endonuclease III: DNA charge transport as a first step in lesion detection.

Authors:  Christine A Romano; Pamela A Sontz; Jacqueline K Barton
Journal:  Biochemistry       Date:  2011-06-09       Impact factor: 3.162

10.  Impaired suppressive activities of human MUTYH variant proteins against oxidative mutagenesis.

Authors:  Kazuya Shinmura; Masanori Goto; Hong Tao; Shun Matsuura; Tomonari Matsuda; Haruhiko Sugimura
Journal:  World J Gastroenterol       Date:  2012-12-21       Impact factor: 5.742
View more

北京卡尤迪生物科技股份有限公司 © 2022-2023.