PLoS ONE (Jan 2022)

Functional characterization of MLH1 missense variants unveils mechanisms of pathogenicity and clarifies role in cancer.

  • Marwa Mahdouani,
  • Slim Ben Ahmed,
  • Fahmi Hmila,
  • Henda Rais,
  • Rihab Ben Sghaier,
  • Hanene Saad,
  • Mariem Ben Said,
  • Saber Masmoudi,
  • Dorra Hmida,
  • Angela Brieger,
  • Stefan Zeuzem,
  • Ali Saad,
  • Moez Gribaa,
  • Guido Plotz

DOI
https://doi.org/10.1371/journal.pone.0278283
Journal volume & issue
Vol. 17, no. 12
p. e0278283

Abstract

Read online

Lynch syndrome is a heritable condition caused by a heterozygous germline inactivating mutation of the DNA mismatch repair (MMR) genes, most commonly the MLH1 gene. However, one third of the identified alterations are missense variants, for which the clinical significance is unclear in many cases. We have identified three MLH1 missense alterations (p.(Glu736Lys), p.(Pro640Thr) and p.(Leu73Pro)) in six individuals from large Tunisian families. For none of these alterations, a classification of pathogenicity was available, consequently diagnosis, predictive testing and targeted surveillance in affected families was impossible. We therefore performed functional laboratory testing using a system testing stability as well as catalytic activity that includes clinically validated reference variants. Both p.(Leu73Pro) and p.(Pro640Thr) were found to be non-functional due to severe defects in protein stability and catalytic activity. In contrast, p.(Glu736Lys) was comparable to the wildtype protein and therefore considered a neutral substitution. Analysis of residue conservation and of the structural roles of the substituted residues corroborated these findings. In conjunction with the available clinical data, two variants fulfil classification criteria for class 4 "likely pathogenic". The findings of this work clarify the mechanism of pathogenicity of two unclear MLH1 variants and enables predictive testing and targeted surveillance in members of carrier families worldwide.