نتایج جستجو برای: ژن mlh3

تعداد نتایج: 15882  

ژورنال: :مجله دانشگاه علوم پزشکی شهید صدوقی یزد 0
حسین پاشایی فر h pashaiefar محمد حسن شیخها mh sheikhha سید مهدی کلانتر m kalantar طاهره جهانی نژآد t jahaninejad محمدعلی زعیمی ma zaimy

مقدمه: حدود نیمی از موارد ناباروری زوجین به علت عوامل مردانه است. آزواسپرمی یا الیگواسپرمی شدید و بدون علت که در نتیجه تغییرات ژنتیکی حاصل می شود، بخش مهمی از ناباروری مردان را تشکیل می دهد. یک مرحله مهم در فرآیند اسپرماتوژنزیس وقایع کراسینگ اور در حین نوترکیبی هومولوگ در تقسیم میوز است. پروتئین mlh3 نقش اساسی در فرآیند نوترکیبی و اسپرماتوژنزیس دارد. این مطالعه به بررسی رابطه یک پلی مورفیسم عمل...

2017
Najla Al-Sweel Vandana Raghavan Abhishek Dutta V P Ajith Luigi Di Vietro Nabila Khondakar Carol M Manhart Jennifer A Surtees K T Nishant Eric Alani

Mlh1-Mlh3 is an endonuclease hypothesized to act in meiosis to resolve double Holliday junctions into crossovers. It also plays a minor role in eukaryotic DNA mismatch repair (MMR). To understand how Mlh1-Mlh3 functions in both meiosis and MMR, we analyzed in baker's yeast 60 new mlh3 alleles. Five alleles specifically disrupted MMR, whereas one (mlh3-32) specifically disrupted meiotic crossing...

Journal: :Cancer research 2005
Peng-Chieh Chen Sandra Dudley Wayne Hagen Diana Dizon Leslie Paxton Denise Reichow Song-Ro Yoon Kan Yang Norman Arnheim R Michael Liskay Steven M Lipkin

Germ line DNA mismatch repair mutations in MLH1 and MSH2 underlie the vast majority of hereditary non-polyposis colon cancer. Four mammalian homologues of Escherichia coli MutL heterodimerize to form three distinct complexes: MLH1/PMS2, MLH1/MLH3, and MLH1/PMS1. Although MLH1/PMS2 is generally thought to have the major MutL activity, the precise contributions of each MutL heterodimer to mismatc...

Journal: :Genetics 2008
K T Nishant Aaron J Plys Eric Alani

Interference-dependent crossing over in yeast and mammalian meioses involves the mismatch repair protein homologs MSH4-MSH5 and MLH1-MLH3. The MLH3 protein contains a highly conserved metal-binding motif DQHA(X)(2)E(X)(4)E that is found in a subset of MLH proteins predicted to have endonuclease activities (Kadyrov et al. 2006). Mutations within this motif in human PMS2 and Saccharomyces cerevis...

2008
K. T. Nishant Aaron J. Plys Eric Alani

Interference-dependent crossing over in yeast and mammalian meioses involves the mismatch repair protein homologs MSH4-MSH5 and MLH1-MLH3. The MLH3 protein contains a highly conserved metal binding motif DQHA(X)2E(X)4E that is found in a subset of MLH proteins predicted to have endonuclease activities (KADYROV et al. 2006). Mutations within this motif in human PMS2 and S. cerevisiae PMS1 disrup...

Journal: :Human molecular genetics 2002
Sabine Santucci-Darmanin Sophie Neyton Françoise Lespinasse Anne Saunières Patrick Gaudray Véronique Paquis-Flucklinger

The mismatch-repair (MMR) system plays a central role in maintaining genetic stability and requires evolutionarily conserved protein factors, including MutS and MutL homologs. Since the discovery of a link between the malfunction of post-replicative MMR and human cancers, a number of works have focused on the function of MutS and MutL homologs in the correction of replication errors. However, s...

Journal: :Genes, chromosomes & cancer 2009
Jianghua Ou Merete Rasmussen Helga Westers Sofie D Andersen Paul O Jager Krista A Kooi Renée C Niessen Bart J L Eggen Finn C Nielsen Jan H Kleibeuker Rolf H Sijmons Lene J Rasmussen Robert M W Hofstra

So far 18 MLH3 germline mutations/variants have been identified in familial colorectal cancer cases. Sixteen of these variants are amino acid substitutions of which the pathogenic nature is still unclear. These substitutions are known as unclassified variants or UVs. To clarify a possible role for eight of these MLH3 UVs identified in suspected Lynch syndrome patients, we performed several bioc...

Journal: :PLoS Genetics 2008
Peng-Chieh Chen Mari Kuraguchi John Velasquez Yuxun Wang Kan Yang Robert Edwards Dan Gillen Winfried Edelmann Raju Kucherlapati Steven M. Lipkin

DNA mismatch repair suppresses gastrointestinal tumorgenesis. Four mammalian E. coli MutL homologues heterodimerize to form three distinct complexes: MLH1/PMS2, MLH1/MLH3, and MLH1/PMS1. To understand the mechanistic contributions of MLH3 and PMS2 in gastrointestinal tumor suppression, we generated Mlh3(-/-);Apc(1638N) and Mlh3(-/-);Pms2(-/-);Apc(1638N) (MPA) mice. Mlh3 nullizygosity significan...

Journal: :Genetics 2008
Anton Svetlanov Frederic Baudat Paula E Cohen Bernard de Massy

The four mammalian MutL homologs (MLH1, MLH3, PMS1, and PMS2) participate in a variety of events, including postreplicative DNA repair, prevention of homeologous recombination, and crossover formation during meiosis. In this latter role, MLH1-MLH3 heterodimers predominate and are essential for prophase I progression. Previous studies demonstrated that mice lacking Mlh1 exhibit a 90% reduction i...

2013
Megan Sonntag Brown Elisha Lim Cheng Chen K. T. Nishant Eric Alani

Crossing over between homologous chromosomes occurs during the prophase of meiosis I and is critical for chromosome segregation. In baker's yeast, two heterodimeric complexes, Msh4-Msh5 and Mlh1-Mlh3, act in meiosis to promote interference-dependent crossing over. Mlh1-Mlh3 also plays a role in DNA mismatch repair (MMR) by interacting with Msh2-Msh3 to repair insertion and deletion mutations. M...

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