hereditary non-polyposis colorectal carcinoma (HNPCC) is associated with early onset carcinoma of colorectum , endometrium, small bowel, renal pelvis and ureter, ovary, hepatobiliary system, brain and skin. 90% of patients with HNPCC have mutations of either MLH1 or MSH2; most of the remainder have mutations of PMS2 or MSH6. HNPCC in women confers a 42% to 60% lifetime probability of developing endometrial carcinoma.
Colonic and endometrial carcinomas in HNPCC can be demonstrated to have MSI. MSI can also be found in 17% to 23% of non-familial endometrial carcinomas: this MSI is attributable to silencing of the MLH1 gene by promoter methylation.
MSI is associated with a favorable clinical outcome in endometrial carcinoma.
MSI can be demonstrated by polymerase chain reaction. However, in routine diagnostic practice, monoclonal antibodies demonstrating loss of staining for at least some MMR gene proteins have good sensitivity and specificity for predicting MSI. Some mutant proteins remain detectable by IHC, giving false results.
For colonic neoplasms:
|
Abnormal (loss of staining) |
MSI-high by PCR |
not MSI-high by PCR |
sensitivity of IHC for MSI |
specificity of IHC for MSI |
||
|
MLH1 |
5/412 |
1/612 |
123%2 |
98%2 |
||
|
MSH2 |
25/402 |
0/622 |
63%2 |
100%2 |
||
|
MSH6 |
20/372 |
0/602 |
54%2 |
100%2 |
||
For endometrial carcinomas:
|
Abnormal (loss of staining) |
MSI-high by PCR |
not MSI-high by PCR |
sensitivity of IHC for MSI |
specificity of IHC for MSI |
||
|
MLH1 |
24/451 |
1/401 |
53%1 |
98%1 |
||
|
PMS2 |
31/451 |
1/401 |
69%1 |
98%1 |
||
|
MSH2 |
7/451 |
0/401 |
18%1 |
100%1 |
||
|
MSH6 |
12/451 |
6/401 |
27%1 |
85%1 |
||
Diagnosis of HNPCC families. As a screening procedure, a four antibody panel gives the highest sensitivity, albeit with reduced specificity.
References
This page last revised 5.6.2007.
©SMUHT/PW Bishop