|
|
|
|
|
|
|
|
|
|
abstract - American Journal of Clinical Pathology
June 29, 2016
Objectives:
Lynch syndrome (LS) predisposes individuals to developing synchronous
and metachronous LS-associated neoplasms (LSANs). Mismatch repair
protein (MMRP) immunohistochemistry (IHC) is widely used to identify LS,
but its utility in patients with synchronous/metachronous lesions has
not been studied. We studied MMRP IHC in patients with LS with more than
one LSAN to provide screening recommendations in patients with
synchronous/metachronous neoplasms.
Methods:
All patients with LS diagnosed at The Ohio State University Wexner
Medical Center from 2009 through 2014 with more than one LSAN and
available tumor tissue for immunostaining were identified. Tumors were
stained for MLH1, MSH2, MSH6, and PMS-2 proteins, and immunoreactivity
was scored as intact or lost.
Results:
Thirteen patients with LS with 29 synchronous and/or metachronous
primary LSANs were identified. Neoplasms involved large and small
intestine (n = 19), ampulla (n = 1), endometrium (n = 1), and skin
(sebaceous neoplasms, n = 8). Nine (69%) of 13 patients showed
concordant MMRP results in all tumors, and four (31%) showed discordant
MMRP results.
Conclusions: LS diagnosis
could have been missed in 31% of the study cases if only the LSAN
exhibiting intact MMRP expression was screened. Accordingly, our
findings support the recommendation to perform LS screening in all
primary, synchronous, and metachronous intestinal and endometrial
cancers if a previous tumor screened intact.
0 comments :
Post a Comment
Your comments?
Note: Only a member of this blog may post a comment.