Hereditary cancer syndrome diagnosis: molecular genetic clues and cancer control

Author:

Lynch Henry T1,Fusaro Ramon M1,Lynch Jane F1

Affiliation:

1. Creighton University School of Medicine, Department of Preventive Medicine 2500, California Plaza Omaha NE 68178, USA.

Abstract

Oncologists who are aware of the progress in hereditary cancer syndrome diagnosis, and, in particular, of how this effort may be effectively facilitated through a comprehensive family history in concert with molecular genetic studies, are in the envious position of designing highly targeted screening and management programs for the membership of these cancer-prone families. The Lynch syndrome is discussed as a clinical model wherein the presence of mismatch repair mutations provides a high level of diagnostic certainty for the initiation of targeted cancer screening and management. The familial atypical multiple mole melanoma–pancreatic cancer (FAMMM–PC) syndrome, on the other hand, provides another model with cancer-control potential. Given its phenotypic features of multiple atypical nevi, high total body mole count and cutaneous malignant melanoma, coupled with the integral association of PC in a subset of FAMMM kindreds with the CDKN2Agermline mutation, this may result in a perhaps lower level of diagnostic certainty when compared with the Lynch syndrome. This knowledge may impact upon progress in the earlier diagnosis of melanoma and provide an impetus for creative diagnostic methods in PC, a disease that, at this time, demonstrates a mortality rate virtually identical to its incidence rate.

Publisher

Future Medicine Ltd

Subject

Cancer Research,Oncology,General Medicine

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