Difference between revisions of "Talk:Lynch syndrome"
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(Created page with "<pre> COLON, RESECTION: - ADENOCARCIOM TUMOUR HAS BEEN EXAMINED FOR THE MISMATCH REPAIR GENE PRODUCTS: MLH1: ABNORMAL, FOCAL MINIMAL STAINING IN THE TUMOUR COMPARED TO BENI...") |
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<pre> | <pre> | ||
COLON, RESECTION: | COLON, RESECTION: | ||
- | - ADENOCARCINOMA. | ||
- TUMOUR HAS BEEN EXAMINED FOR THE MISMATCH REPAIR GENE PRODUCTS. | |||
MLH1: ABNORMAL, FOCAL MINIMAL STAINING IN THE TUMOUR COMPARED TO BENIGN BACKGROUND CELLS. | |||
MSH2: NORMAL NUCLEAR STAINING. | |||
MSH6: NORMAL NUCLEAR STAINING. | |||
PMS2: ABNORMAL, ABSENT NUCLEAR STAINING, SEE COMMENT. | |||
COMMENT: | |||
Abnormal immunohistochemical staining is highly correlated (>99%) with tumours that | |||
show high-frequency microsatellite instability (MSI-H) and this tumour should be | |||
consider to have microsatellite instability (MSI-H). | |||
The MLH1 staining is abnormal; it is very week and focal in the lesion, when compared | |||
to the background tissues. PMS2 is completely absent. | |||
The expression of PMS2 is lost in tumours with abnormal MLH1 expression. As the MLH1 | |||
is decreased but not completely absent, this individual's PMS2 status cannot be determined | |||
by immunohistochemistry, and the individual could be considered for furthe investigation | |||
of MLH1 status. | |||
Abnormal MLH1 expression can be seen in sporadic tumours (associated with MLH1 | |||
hypermethylation) as well as in association with Lynch syndrome (LS), also known as | |||
hereditary non-polyposis colon cancer (HNPCC). Features associated with LS include young | |||
age of onset, strong family history of cancer (especially endometrial, urothelial, other | |||
gastrointestinal), and multiple primary LS cancers in one individual. If this patient | |||
has these characteristics suggestive of LS, a referral to a genetic counsellor | |||
is suggested. | |||
</pre> | </pre> | ||
Latest revision as of 21:43, 16 December 2013
COLON, RESECTION:
- ADENOCARCINOMA.
- TUMOUR HAS BEEN EXAMINED FOR THE MISMATCH REPAIR GENE PRODUCTS.
MLH1: ABNORMAL, FOCAL MINIMAL STAINING IN THE TUMOUR COMPARED TO BENIGN BACKGROUND CELLS.
MSH2: NORMAL NUCLEAR STAINING.
MSH6: NORMAL NUCLEAR STAINING.
PMS2: ABNORMAL, ABSENT NUCLEAR STAINING, SEE COMMENT.
COMMENT:
Abnormal immunohistochemical staining is highly correlated (>99%) with tumours that
show high-frequency microsatellite instability (MSI-H) and this tumour should be
consider to have microsatellite instability (MSI-H).
The MLH1 staining is abnormal; it is very week and focal in the lesion, when compared
to the background tissues. PMS2 is completely absent.
The expression of PMS2 is lost in tumours with abnormal MLH1 expression. As the MLH1
is decreased but not completely absent, this individual's PMS2 status cannot be determined
by immunohistochemistry, and the individual could be considered for furthe investigation
of MLH1 status.
Abnormal MLH1 expression can be seen in sporadic tumours (associated with MLH1
hypermethylation) as well as in association with Lynch syndrome (LS), also known as
hereditary non-polyposis colon cancer (HNPCC). Features associated with LS include young
age of onset, strong family history of cancer (especially endometrial, urothelial, other
gastrointestinal), and multiple primary LS cancers in one individual. If this patient
has these characteristics suggestive of LS, a referral to a genetic counsellor
is suggested.