Biochemical characterization of MLH3 missense mutations does not reveal an apparent role of MLH3 in Lynch syndrome

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

doi:10.1002/gcc.20644

Biochemical characterization of MLH3 missense mutations does not reveal an apparent role of MLH3 in Lynch syndrome

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

14 Citations (Scopus)

Abstract

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 biochemical tests. We determined the protein expression and stability, protein localization and interaction of the mutant MLH3 proteins with wildtype MLH1. All eight MLH3 UVs gave protein expression levels comparable with wildtype MLH3. Furthermore, the UV-containing proteins, in contrast to previous studies, were all localized normally in the nucleus and they interacted normally with wildtype MLH1. Our different biochemical assays yielded no evidence that the eight MLH3 UVs tested are the cause of hereditary colorectal cancer, including Lynch syndrome.

Original language	English
Journal	Genes, Chromosomes & Cancer
Volume	48
Issue number	4
Pages (from-to)	340-50
Number of pages	10
ISSN	1045-2257
DOIs	https://doi.org/10.1002/gcc.20644
Publication status	Published - 2009

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Ou, J., Rasmussen, M., Westers, H., Andersen, S. D., Jager, P. O., Kooi, K. A., Niessen, R. C., Eggen, B. J. L., Nielsen, F. C., Kleibeuker, J. H., Sijmons, R. H., Rasmussen, L. J., & Hofstra, R. M. W. (2009). Biochemical characterization of MLH3 missense mutations does not reveal an apparent role of MLH3 in Lynch syndrome. Genes, Chromosomes & Cancer, 48(4), 340-50. https://doi.org/10.1002/gcc.20644

Ou, J, Rasmussen, M, Westers, H, Andersen, SD, Jager, PO, Kooi, KA, Niessen, RC, Eggen, BJL, Nielsen, FC, Kleibeuker, JH, Sijmons, RH, Rasmussen, LJ & Hofstra, RMW 2009, 'Biochemical characterization of MLH3 missense mutations does not reveal an apparent role of MLH3 in Lynch syndrome', Genes, Chromosomes & Cancer, vol. 48, no. 4, pp. 340-50. https://doi.org/10.1002/gcc.20644

@article{1f601c706a4e11df928f000ea68e967b,

title = "Biochemical characterization of MLH3 missense mutations does not reveal an apparent role of MLH3 in Lynch syndrome",

abstract = "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 biochemical tests. We determined the protein expression and stability, protein localization and interaction of the mutant MLH3 proteins with wildtype MLH1. All eight MLH3 UVs gave protein expression levels comparable with wildtype MLH3. Furthermore, the UV-containing proteins, in contrast to previous studies, were all localized normally in the nucleus and they interacted normally with wildtype MLH1. Our different biochemical assays yielded no evidence that the eight MLH3 UVs tested are the cause of hereditary colorectal cancer, including Lynch syndrome.",

author = "Jianghua Ou and Merete Rasmussen and Helga Westers and Andersen, {Sofie D} and Jager, {Paul O} and Kooi, {Krista A} and Niessen, {Ren{\'e}e C} and Eggen, {Bart J L} and Nielsen, {Finn C} and Kleibeuker, {Jan H} and Sijmons, {Rolf H} and Rasmussen, {Lene J} and Hofstra, {Robert M W}",

note = "Keywords: Adaptor Proteins, Signal Transducing; Amino Acid Sequence; Carrier Proteins; Cell Line; Colorectal Neoplasms, Hereditary Nonpolyposis; Computer Simulation; DNA Mutational Analysis; Humans; Molecular Sequence Data; Mutation, Missense; Nuclear Proteins; Protein Transport; Sequence Alignment; Two-Hybrid System Techniques",

year = "2009",

doi = "10.1002/gcc.20644",

language = "English",

volume = "48",

pages = "340--50",

journal = "Genes, Chromosomes & Cancer",

issn = "1045-2257",

publisher = "JohnWiley & Sons, Inc.",

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TY - JOUR

T1 - Biochemical characterization of MLH3 missense mutations does not reveal an apparent role of MLH3 in Lynch syndrome

AU - Ou, Jianghua

AU - Rasmussen, Merete

AU - Westers, Helga

AU - Andersen, Sofie D

AU - Jager, Paul O

AU - Kooi, Krista A

AU - Niessen, Renée C

AU - Eggen, Bart J L

AU - Nielsen, Finn C

AU - Kleibeuker, Jan H

AU - Sijmons, Rolf H

AU - Rasmussen, Lene J

AU - Hofstra, Robert M W

N1 - Keywords: Adaptor Proteins, Signal Transducing; Amino Acid Sequence; Carrier Proteins; Cell Line; Colorectal Neoplasms, Hereditary Nonpolyposis; Computer Simulation; DNA Mutational Analysis; Humans; Molecular Sequence Data; Mutation, Missense; Nuclear Proteins; Protein Transport; Sequence Alignment; Two-Hybrid System Techniques

PY - 2009

Y1 - 2009

N2 - 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 biochemical tests. We determined the protein expression and stability, protein localization and interaction of the mutant MLH3 proteins with wildtype MLH1. All eight MLH3 UVs gave protein expression levels comparable with wildtype MLH3. Furthermore, the UV-containing proteins, in contrast to previous studies, were all localized normally in the nucleus and they interacted normally with wildtype MLH1. Our different biochemical assays yielded no evidence that the eight MLH3 UVs tested are the cause of hereditary colorectal cancer, including Lynch syndrome.

AB - 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 biochemical tests. We determined the protein expression and stability, protein localization and interaction of the mutant MLH3 proteins with wildtype MLH1. All eight MLH3 UVs gave protein expression levels comparable with wildtype MLH3. Furthermore, the UV-containing proteins, in contrast to previous studies, were all localized normally in the nucleus and they interacted normally with wildtype MLH1. Our different biochemical assays yielded no evidence that the eight MLH3 UVs tested are the cause of hereditary colorectal cancer, including Lynch syndrome.

U2 - 10.1002/gcc.20644

DO - 10.1002/gcc.20644

M3 - Journal article

C2 - 19156873

SN - 1045-2257

VL - 48

SP - 340

EP - 350

JO - Genes, Chromosomes & Cancer

JF - Genes, Chromosomes & Cancer

IS - 4

ER -

Biochemical characterization of MLH3 missense mutations does not reveal an apparent role of MLH3 in Lynch syndrome

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