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Analysis of families with Lynch syndrome complicated by advanced serrated neoplasia: the importance of pathology review and pedigree analysis |
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| Authors: | Michael D Walsh Daniel D Buchanan Rhiannon Walters Aedan Roberts Sven Arnold Diane McKeone Mark Clendenning Andrew R Ruszkiewicz Mark A Jenkins John L Hopper Jack Goldblatt Jillian George Graeme K Suthers Kerry Phillips Graeme P Young Finlay Macrae Musa Drini Michael O Woods Susan Parry Jeremy R Jass Joanne P Young |
| Institution: | 1. Familial Cancer Laboratory, QIMR, Herston, QLD, 4006, Australia 2. School of Medicine, University of Queensland, Herston, QLD, 4006, Australia 3. Institute of Medical and Veterinary Science, Adelaide, SA, 5000, Australia 4. Centre for MEGA, School of Population Health, University of Melbourne, Carlton, VIC, 3053, Australia 5. Genetic Services of Western Australia, Subiaco, WA, 6008, Australia 6. School of Paediatrics and Child Health University of Western Australia, Nedlands, WA, 6009, Australia 7. South Australian Clinical Genetics Service, North Adelaide, SA, 5009, Australia 8. Department of Paediatrics, University of Adelaide, Adelaide, SA, 5005, Australia 9. Department of Medicine, Flinders University, Bedford Park, SA, 5042, Australia 10. Department of Colorectal Medicine and Genetics, The Royal Melbourne Hospital, Parkville, VIC, 3050, Australia 11. Discipline of Genetics, Faculty of Medicine, Memorial University of Newfoundland, St. John’s, NL, A1C 5S, Canada 12. Department of Gastroenterology, Middlemore Hospital, Auckland, New Zealand 13. Department of Cellular Pathology, St. Mark’s Hospital, Harrow, HA1 3UJ, UK |
| Abstract: | The identification of Lynch syndrome has been greatly assisted by the advent of tumour immunohistochemistry (IHC) for mismatch repair (MMR) proteins, and by the recognition of the role of acquired somatic BRAF mutation in sporadic MMR-deficient colorectal cancer (CRC). However, somatic BRAF mutation may also be present in the tumours in families with a predisposition to develop serrated polyps in the colorectum. In a subgroup of affected members in these families, CRCs emerge which demonstrate clear evidence of MMR deficiency with absent MLH1 staining and high-level microsatellite instability (MSI). This may result in these families being erroneously classified as Lynch syndrome, or conversely, an individual is considered “sporadic” due to the presence of a somatic BRAF mutation in a tumour. In this report, we describe two Lynch syndrome families who demonstrated several such inconsistencies. In one family, IHC deficiency of both MSH2 and MLH1 was demonstrated in tumours from different affected family members, presenting a confusing diagnostic picture. In the second family, MLH1 loss was observed in the lesions of both MLH1 mutation carriers and those who showed normal MLH1 germline sequence. Both families had Lynch syndrome complicated by an independently segregating serrated neoplasia phenotype, suggesting that in families such as these, tumour and germline studies of several key members, rather than of a single proband, are indicated to clarify the spectrum of risk. |
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