Ten novel MSH2 and MLH1 germline mutations in families with HNPCC.

Publikation: Beitrag in FachzeitschriftForschungsartikelBeigetragenBegutachtung

Beitragende

  • Stefan Krüger - , Abteilung Chirurgische Forschung (Autor:in)
  • Andrea Bier - , Abteilung Chirurgische Forschung, Institut für Klinische Genetik (Autor:in)
  • Jens Plaschke - , Abteilung Chirurgische Forschung (Autor:in)
  • Ruth Höhl - , Abteilung Chirurgische Forschung (Autor:in)
  • Daniela E. Aust - , Institut für Pathologie, Universitätsklinikum Carl Gustav Carus Dresden (Autor:in)
  • Friedmar R. Kreuz - , Institut für Klinische Genetik (Autor:in)
  • Steffen R. Pistorius - , Klinik und Poliklinik für Viszeral- Thorax- und Gefäßchirurgie, Universitätsklinikum Carl Gustav Carus Dresden (Autor:in)
  • Hans D. Saeger - , Klinik und Poliklinik für Viszeral-, Thorax- und Gefäßchirurgie (Autor:in)
  • Veit Rothhammer - , Universitätsklinikum Carl Gustav Carus Dresden (Autor:in)
  • Oliver Al-Taie - , Universitätsklinikum Carl Gustav Carus Dresden (Autor:in)
  • Hans K. Schackert - , Abteilung Chirurgische Forschung (Autor:in)

Abstract

Hereditary nonpolyposis colorectal cancer (HNPCC) is one of the most common hereditary cancer-susceptibility syndromes. Germline mutations in mismatch repair genes are associated with the clinical phenotype of HNPCC. We report ten novel germline mutations, three in MSH2 and seven in MLH1. All but one mutation have been found in families fulfilling criteria of the Bethesda guidelines; four of them additionally fulfilled the Amsterdam criteria I or II. Eight mutations were considered pathogenic and predictive diagnostics in healthy family members at risk shall be undertaken; these include five frameshift mutations leading to premature stop codons, in MSH2: c.1672delT (p.S558Xfs) and c.2466_2467delTG (p.C822X) and in MLH1: c.1023delG (p.R341Xfs), c.1127_1128dupAT (p.K377Xfs) and c.1310delC (p.P437Xfs); three mutations leading to splice aberrations, in MSH2: c.1661G>C (r.1511_1661del) and in MLH1: c.677+3A>C (r.589_677del) and c.1990-2A>G predicted to result in a splice site defect. The remaining two mutations are unclassified variants with assumed pathogenicity: one missense mutation in the highly conserved ATPase domain of MLH1 (c.122A>G [p.D41G]) and one in-frame insertion of twelve nucleotides in MLH1 (c.2155_2156insATGTGTTCCACA [p.I719delinsNVFHI]). These two mutations were not found in 102 alleles of healthy control individuals. The corresponding tumors from all patients showed a high level of microsatellite instability (MSI-H). Immunohistochemistry (IHC) revealed complete loss of expression of the affected protein in the tumor cells from all but three patients. The tumors from the patients with the mutations c.1127_1128dupAT and c.1990-2A>G showed a reduction of expression of the MLH1-protein, rather than complete loss. In the tumor from the patient with the missense mutation c.122A>G [p.D41G] a normal expression of the proteins coded by MLH1 and MSH2 was noticed.

Details

OriginalspracheEnglisch
Seiten (von - bis)351-352
Seitenumfang2
FachzeitschriftHuman mutation
Jahrgang24
Ausgabenummer4
PublikationsstatusVeröffentlicht - Okt. 2004
Peer-Review-StatusJa

Externe IDs

PubMed 15365996

Schlagworte

Ziele für nachhaltige Entwicklung

ASJC Scopus Sachgebiete