Table 1. Variants identified in the hMLH1 and hMSH2 genes during this study.
| Gene | Family ID | Risk statusa | MSI | Exon | Nucleotide | Effect | Types of cancer |
|---|---|---|---|---|---|---|---|
| Mutation | |||||||
| hMLH1 | 3335 | Amsterdam | 4/5 | 15 | 1669G>T b | E557X | CRCc, melanoma, liver, TCCd, endometrium, lung |
| 5838 | Amsterdam | NT | 8 | 676C>T | R226X | CRCc, endometrium, larynx, stomach | |
| hMSH2 | 7562 | Amsterdam | 0/5 | 3 | Dele 2.2 kb | Protein missing aa 123–215 | CRCc, endometrium |
| 8344 | Bethesda | 4/5 | 3 | 472C>T b | Q158X | CRCc | |
| 8902 | Amsterdam | 5/5 | 13 | 2131C>T | R711X | CRCc, ovaries, endometrium | |
| 9663 | Amsterdam | NT | 11 | 1704_1705dele AGb | Fsf resulting in STOP at codon 570 | CRCc, endometrium | |
| 10107 | Amsterdam | NT | 6 | 1076G>T b | R359X | CRCc, ovary, endometrium, urinary tract, eye, prostate, melanoma, breast | |
| Gene | Exon | Codon | Nucleotide change | Consequences | No. of families | ||
| Benign polymorphisms | |||||||
| hMLH1 | IVS 4 | 309−30 b | c>a | — | 2 | ||
| Exon 8 | 219 | 655A>G | I219V | 5 | |||
| Exon 12 | 464 b | 464T>C | P464P | ||||
| IVS 12 | 1408−54 b | c>t | — | 2 | |||
| IVS 13 | 1558−13 | g>a | — | 2 | |||
| IVS 14 | 1668−19 | a>g | 6 | ||||
| hMSH2 | IVS 1 | 211+9 | c>g | — | 1 | ||
| Exon 4 | 224 b | 669C>T | L224L | 2 | |||
| IVS 9 | 1511−9 | a>t | — | 1 | |||
| IVS 10 | 1661+13 | g>a | — | 2 | |||
| IVS 12 | 2006−6 | t>c | — | 2 | |||
a
Risk status based on the Amsterdam II (Vasen et al, 1999) and Bethesda (Rodrigues – Bigas et al, 1997) criteria.
b
Novel variations identified in this study (marked in bold).
c
CRC=colorectal cancer.
d
TCC=transitional cell carcinoma.
e
Del=deletion.
f
Fs=frame shift mutation.