Reduced mRNA expression in paraffin-embedded tissue identifies MLH1- and MSH2-deficient colorectal tumours and potential mutation carriers

Annegret Müller; Dirk Zielinski; Nicolaus Friedrichs; Barbara Oberschmid; Sabine Merkelbach-Bruse; Hans K. Schackert; Markus Linnebacher; Magnus Von Knebel Doeberitz; Reinhard Büttner; Josef Rüschoff; K. Schulmann; F. E. Brasch; J. T. Epplen; K. M. Müller; C. Pox; S. Stemmler; J. Willert; W. Friedl; J. Girmscheid; A. Hirner; C. Lamberti; M. Mathiak; P. Propping; T. Sauerbruch; K. Siberg; G. Moeslein; T. Goecke; A. Hansmann; S. Höwer; C. Poremba; A. Unger; C. Wieland; D. Aust; F. Balck; R. Höhl; S. Krüger; E. Schröck; S. Pistorius; F. Cremer; J. Gebert; M. Keller; P. Kienle; M. Kloor; U. Mazitschek; M. Tariverdian; I. Becker; E. Holinski-Feder; G. Keller; R. Kopp; Y. Müller-Koch; K. Ott; P. Rümmele; J. Forberg; M. Herold; M. Loeffler; J. Schaefer; R. Speer

doi:10.1007/s00428-008-0637-2

Reduced mRNA expression in paraffin-embedded tissue identifies MLH1- and MSH2-deficient colorectal tumours and potential mutation carriers

Annegret Müller, Dirk Zielinski, Nicolaus Friedrichs, Barbara Oberschmid, Sabine Merkelbach-Bruse, Hans K. Schackert, Markus Linnebacher, Magnus Von Knebel Doeberitz, Reinhard Büttner, Josef Rüschoff, K. Schulmann, F. E. Brasch, J. T. Epplen, K. M. Müller, C. Pox, S. Stemmler, J. Willert, W. Friedl, J. Girmscheid, A. HirnerC. Lamberti, M. Mathiak, P. Propping, T. Sauerbruch, K. Siberg, G. Moeslein, T. Goecke, A. Hansmann, S. Höwer, C. Poremba, A. Unger, C. Wieland, D. Aust, F. Balck, R. Höhl, S. Krüger, E. Schröck, S. Pistorius, F. Cremer, J. Gebert, M. Keller, P. Kienle, M. Kloor, U. Mazitschek, M. Tariverdian, I. Becker, E. Holinski-Feder, G. Keller, R. Kopp, Y. Müller-Koch, K. Ott, P. Rümmele, J. Forberg, M. Herold, M. Loeffler, J. Schaefer, R. Speer

Medicine and Health

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Abstract

Based on the principle of nonsense-mediated mRNA decay, we sought to identify MLH1 or MSH2-deficient colorectal tumours through relative quantification of mRNA expression with real-time PCR (RT-PCR) analysis. MLH1 and MSH2 mRNAs were almost equally expressed as defined by MLH1 to MSH2 transcript ratio (mean 1.41) in microsatellite stable, mismatch repair (MMR) proficient tumours (n=16). A close correlation between loss of protein expression and MMR-mRNA levels was found in highly microsatellite instable (MSI-H) tumours deficient of MLH1 or MSH2. MLH1/MSH2 ratio was low in 11 sporadic and nine hereditary MLH1-deficient carcinomas (mean 0.51), whereas the ratio was high in 17 MSH2-deficient hereditary non-polyposis colorectal cancer (HNPCC) associated carcinomas (mean 6.8). Notably, in the normal tissues of HNPCC patients with MSH2 mutations, the MLH1/MSH2 transcript ratios were significantly elevated (ratio>2.0) as compared to the ratios of normal mucosa in patients with MMR-proficient tumours (27 of 32 ratio<2.0; p=0.00113). Analysis of B-lymphocytes of HNPCC patients with proven MMR gene mutation confirmed these findings. In conclusion, RT-PCR allows relative quantification of MMR gene mRNA expression in formalin-fixed and paraffin-embedded tissue. Furthermore, this approach enables quantification of haploinsufficiency due to nonsense-mediated mRNA decay in normal tissue and B-lymphocytes from patients carrying MSH2 germline mutations and may be useful for identification of asymptomatic carriers of pathogenic germline mutations.

Original language	English
Pages (from-to)	9-16
Number of pages	8
Journal	Virchows Archiv
Volume	453
Issue number	1
DOIs	https://doi.org/10.1007/s00428-008-0637-2
State	Published - Jul 2008

Keywords

Diagnostic tool
MMR-deficient tumours
Nonsense-mediated decay
qRT-PCR

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1007/s00428-008-0637-2

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Müller, A., Zielinski, D., Friedrichs, N., Oberschmid, B., Merkelbach-Bruse, S., Schackert, H. K., Linnebacher, M., Von Knebel Doeberitz, M., Büttner, R., Rüschoff, J., Schulmann, K., Brasch, F. E., Epplen, J. T., Müller, K. M., Pox, C., Stemmler, S., Willert, J., Friedl, W., Girmscheid, J., ... Speer, R. (2008). Reduced mRNA expression in paraffin-embedded tissue identifies MLH1- and MSH2-deficient colorectal tumours and potential mutation carriers. Virchows Archiv, 453(1), 9-16. https://doi.org/10.1007/s00428-008-0637-2

@article{27b5e5a9c41b41418c6df74ec515c654,

title = "Reduced mRNA expression in paraffin-embedded tissue identifies MLH1- and MSH2-deficient colorectal tumours and potential mutation carriers",

abstract = "Based on the principle of nonsense-mediated mRNA decay, we sought to identify MLH1 or MSH2-deficient colorectal tumours through relative quantification of mRNA expression with real-time PCR (RT-PCR) analysis. MLH1 and MSH2 mRNAs were almost equally expressed as defined by MLH1 to MSH2 transcript ratio (mean 1.41) in microsatellite stable, mismatch repair (MMR) proficient tumours (n=16). A close correlation between loss of protein expression and MMR-mRNA levels was found in highly microsatellite instable (MSI-H) tumours deficient of MLH1 or MSH2. MLH1/MSH2 ratio was low in 11 sporadic and nine hereditary MLH1-deficient carcinomas (mean 0.51), whereas the ratio was high in 17 MSH2-deficient hereditary non-polyposis colorectal cancer (HNPCC) associated carcinomas (mean 6.8). Notably, in the normal tissues of HNPCC patients with MSH2 mutations, the MLH1/MSH2 transcript ratios were significantly elevated (ratio>2.0) as compared to the ratios of normal mucosa in patients with MMR-proficient tumours (27 of 32 ratio<2.0; p=0.00113). Analysis of B-lymphocytes of HNPCC patients with proven MMR gene mutation confirmed these findings. In conclusion, RT-PCR allows relative quantification of MMR gene mRNA expression in formalin-fixed and paraffin-embedded tissue. Furthermore, this approach enables quantification of haploinsufficiency due to nonsense-mediated mRNA decay in normal tissue and B-lymphocytes from patients carrying MSH2 germline mutations and may be useful for identification of asymptomatic carriers of pathogenic germline mutations.",

keywords = "Diagnostic tool, MMR-deficient tumours, Nonsense-mediated decay, qRT-PCR",

author = "Annegret M{\"u}ller and Dirk Zielinski and Nicolaus Friedrichs and Barbara Oberschmid and Sabine Merkelbach-Bruse and Schackert, \{Hans K.\} and Markus Linnebacher and \{Von Knebel Doeberitz\}, Magnus and Reinhard B{\"u}ttner and Josef R{\"u}schoff and K. Schulmann and Brasch, \{F. E.\} and Epplen, \{J. T.\} and M{\"u}ller, \{K. M.\} and C. Pox and S. Stemmler and J. Willert and W. Friedl and J. Girmscheid and A. Hirner and C. Lamberti and M. Mathiak and P. Propping and T. Sauerbruch and K. Siberg and G. Moeslein and T. Goecke and A. Hansmann and S. H{\"o}wer and C. Poremba and A. Unger and C. Wieland and D. Aust and F. Balck and R. H{\"o}hl and S. Kr{\"u}ger and E. Schr{\"o}ck and S. Pistorius and F. Cremer and J. Gebert and M. Keller and P. Kienle and M. Kloor and U. Mazitschek and M. Tariverdian and I. Becker and E. Holinski-Feder and G. Keller and R. Kopp and Y. M{\"u}ller-Koch and K. Ott and P. R{\"u}mmele and J. Forberg and M. Herold and M. Loeffler and J. Schaefer and R. Speer",

note = "Funding Information: This work is also supported by the DFG-Grand 1304 (Klinische Forschergruppe 179) Funding Information: Acknowledgements The work of the Consortium is supported by a multi-center grant from the Deutsche Krebshilfe (German Cancer Aid), Bonn, Germany. This study is in part the diploma thesis of D.Z. We thank Katja Br{\"a}utigam and Katja Goldacker for excellent technical assistance.",

year = "2008",

month = jul,

doi = "10.1007/s00428-008-0637-2",

language = "English",

volume = "453",

pages = "9--16",

journal = "Virchows Archiv",

issn = "0945-6317",

number = "1",

}

Müller, A, Zielinski, D, Friedrichs, N, Oberschmid, B, Merkelbach-Bruse, S, Schackert, HK, Linnebacher, M, Von Knebel Doeberitz, M, Büttner, R, Rüschoff, J, Schulmann, K, Brasch, FE, Epplen, JT, Müller, KM, Pox, C, Stemmler, S, Willert, J, Friedl, W, Girmscheid, J, Hirner, A, Lamberti, C, Mathiak, M, Propping, P, Sauerbruch, T, Siberg, K, Moeslein, G, Goecke, T, Hansmann, A, Höwer, S, Poremba, C, Unger, A, Wieland, C, Aust, D, Balck, F, Höhl, R, Krüger, S, Schröck, E, Pistorius, S, Cremer, F, Gebert, J, Keller, M, Kienle, P, Kloor, M, Mazitschek, U, Tariverdian, M, Becker, I, Holinski-Feder, E, Keller, G, Kopp, R, Müller-Koch, Y, Ott, K, Rümmele, P, Forberg, J, Herold, M, Loeffler, M, Schaefer, J & Speer, R 2008, 'Reduced mRNA expression in paraffin-embedded tissue identifies MLH1- and MSH2-deficient colorectal tumours and potential mutation carriers', Virchows Archiv, vol. 453, no. 1, pp. 9-16. https://doi.org/10.1007/s00428-008-0637-2

TY - JOUR

T1 - Reduced mRNA expression in paraffin-embedded tissue identifies MLH1- and MSH2-deficient colorectal tumours and potential mutation carriers

AU - Müller, Annegret

AU - Zielinski, Dirk

AU - Friedrichs, Nicolaus

AU - Oberschmid, Barbara

AU - Merkelbach-Bruse, Sabine

AU - Schackert, Hans K.

AU - Linnebacher, Markus

AU - Von Knebel Doeberitz, Magnus

AU - Büttner, Reinhard

AU - Rüschoff, Josef

AU - Schulmann, K.

AU - Brasch, F. E.

AU - Epplen, J. T.

AU - Müller, K. M.

AU - Pox, C.

AU - Stemmler, S.

AU - Willert, J.

AU - Friedl, W.

AU - Girmscheid, J.

AU - Hirner, A.

AU - Lamberti, C.

AU - Mathiak, M.

AU - Propping, P.

AU - Sauerbruch, T.

AU - Siberg, K.

AU - Moeslein, G.

AU - Goecke, T.

AU - Hansmann, A.

AU - Höwer, S.

AU - Poremba, C.

AU - Unger, A.

AU - Wieland, C.

AU - Aust, D.

AU - Balck, F.

AU - Höhl, R.

AU - Krüger, S.

AU - Schröck, E.

AU - Pistorius, S.

AU - Cremer, F.

AU - Gebert, J.

AU - Keller, M.

AU - Kienle, P.

AU - Kloor, M.

AU - Mazitschek, U.

AU - Tariverdian, M.

AU - Becker, I.

AU - Holinski-Feder, E.

AU - Keller, G.

AU - Kopp, R.

AU - Müller-Koch, Y.

AU - Ott, K.

AU - Rümmele, P.

AU - Forberg, J.

AU - Herold, M.

AU - Loeffler, M.

AU - Schaefer, J.

AU - Speer, R.

N1 - Funding Information: This work is also supported by the DFG-Grand 1304 (Klinische Forschergruppe 179) Funding Information: Acknowledgements The work of the Consortium is supported by a multi-center grant from the Deutsche Krebshilfe (German Cancer Aid), Bonn, Germany. This study is in part the diploma thesis of D.Z. We thank Katja Bräutigam and Katja Goldacker for excellent technical assistance.

PY - 2008/7

Y1 - 2008/7

N2 - Based on the principle of nonsense-mediated mRNA decay, we sought to identify MLH1 or MSH2-deficient colorectal tumours through relative quantification of mRNA expression with real-time PCR (RT-PCR) analysis. MLH1 and MSH2 mRNAs were almost equally expressed as defined by MLH1 to MSH2 transcript ratio (mean 1.41) in microsatellite stable, mismatch repair (MMR) proficient tumours (n=16). A close correlation between loss of protein expression and MMR-mRNA levels was found in highly microsatellite instable (MSI-H) tumours deficient of MLH1 or MSH2. MLH1/MSH2 ratio was low in 11 sporadic and nine hereditary MLH1-deficient carcinomas (mean 0.51), whereas the ratio was high in 17 MSH2-deficient hereditary non-polyposis colorectal cancer (HNPCC) associated carcinomas (mean 6.8). Notably, in the normal tissues of HNPCC patients with MSH2 mutations, the MLH1/MSH2 transcript ratios were significantly elevated (ratio>2.0) as compared to the ratios of normal mucosa in patients with MMR-proficient tumours (27 of 32 ratio<2.0; p=0.00113). Analysis of B-lymphocytes of HNPCC patients with proven MMR gene mutation confirmed these findings. In conclusion, RT-PCR allows relative quantification of MMR gene mRNA expression in formalin-fixed and paraffin-embedded tissue. Furthermore, this approach enables quantification of haploinsufficiency due to nonsense-mediated mRNA decay in normal tissue and B-lymphocytes from patients carrying MSH2 germline mutations and may be useful for identification of asymptomatic carriers of pathogenic germline mutations.

AB - Based on the principle of nonsense-mediated mRNA decay, we sought to identify MLH1 or MSH2-deficient colorectal tumours through relative quantification of mRNA expression with real-time PCR (RT-PCR) analysis. MLH1 and MSH2 mRNAs were almost equally expressed as defined by MLH1 to MSH2 transcript ratio (mean 1.41) in microsatellite stable, mismatch repair (MMR) proficient tumours (n=16). A close correlation between loss of protein expression and MMR-mRNA levels was found in highly microsatellite instable (MSI-H) tumours deficient of MLH1 or MSH2. MLH1/MSH2 ratio was low in 11 sporadic and nine hereditary MLH1-deficient carcinomas (mean 0.51), whereas the ratio was high in 17 MSH2-deficient hereditary non-polyposis colorectal cancer (HNPCC) associated carcinomas (mean 6.8). Notably, in the normal tissues of HNPCC patients with MSH2 mutations, the MLH1/MSH2 transcript ratios were significantly elevated (ratio>2.0) as compared to the ratios of normal mucosa in patients with MMR-proficient tumours (27 of 32 ratio<2.0; p=0.00113). Analysis of B-lymphocytes of HNPCC patients with proven MMR gene mutation confirmed these findings. In conclusion, RT-PCR allows relative quantification of MMR gene mRNA expression in formalin-fixed and paraffin-embedded tissue. Furthermore, this approach enables quantification of haploinsufficiency due to nonsense-mediated mRNA decay in normal tissue and B-lymphocytes from patients carrying MSH2 germline mutations and may be useful for identification of asymptomatic carriers of pathogenic germline mutations.

KW - Diagnostic tool

KW - MMR-deficient tumours

KW - Nonsense-mediated decay

KW - qRT-PCR

UR - http://www.scopus.com/inward/record.url?scp=48349143473&partnerID=8YFLogxK

U2 - 10.1007/s00428-008-0637-2

DO - 10.1007/s00428-008-0637-2

M3 - Article

C2 - 18581137

AN - SCOPUS:48349143473

SN - 0945-6317

VL - 453

SP - 9

EP - 16

JO - Virchows Archiv

JF - Virchows Archiv

IS - 1

ER -

Reduced mRNA expression in paraffin-embedded tissue identifies MLH1- and MSH2-deficient colorectal tumours and potential mutation carriers

Abstract

Keywords

UN SDGs

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