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Abstract
Studies have suggested serous tubal intraepithelial carcinoma
(STIC) of the fallopian tube to be a putative precursor to ovarian and
peritoneal serous carcinoma. It has been recommended that resected
fallopian tube specimens should be rigorously examined for STIC,
especially in women at high risk of serous carcinoma, such as those with
BRCA mutations or with a strong family history. The SEE-FIM
protocol allows for the greatest surface area of the tube to be
histologically assessed. There have been suggestions that multiple
deeper sections should be examined if the initial hematoxylin and eosin
(H&E) sections are negative; however, whether this identifies more
cases of STIC has not rigorously examined. We examined deeper sections
from 56 cases of pelvic carcinoma in which the initial H&E sections
of the fallopian tubes were negative for STIC. All initial and deeper
sections underwent consensus review by panel of experts in gynecologic
pathology. These cases are part of a larger study in which we had
examined 300 consecutive bilateral salpingectomies using the SEE-FIM
protocol and a single-H&E section per block and had identified 68
cases of pelvic serous carcinoma, of which 12 were associated with STIC.
We calculated the sensitivity of a single-H&E section to detect
STIC, as compared with examination of multiple deeper sections, and
reevaluated the clinicopathologic data of the parent study in light of
the additional cases of STIC. In the 56 cases initially negative for
STIC, 4 cases of STIC were identified after examination of multiple
deeper sections of the fallopian tubes. The single-H&E section
SEE-FIM approach therefore detected only 75% (95% confidence interval,
51%–90%) of STIC that was present. Three of these new cases were
associated with primary ovarian serous carcinoma and 1 with primary
peritoneal serous carcinoma. All 3 new cases associated with ovarian
carcinoma were noted in women without neoadjuvant chemotherapy. In
considering the data from the parent study, we calculated a
statistically significant lower incidence of STIC in women with ovarian
serous carcinoma who received neoadjuvant chemotherapy as compared with
those who did not (P=0.042). Our study demonstrated that
additional cases of STIC can be detected if deeper sections are
examined. These additional cases also highlighted a statistically
significant difference in the incidence of STIC associated with ovarian
serous carcinoma who received neoadjuvant chemotherapy relative to those
who did not. Consideration to this should be given in future studies of
the prevalence of STIC and to routine examination of salpingectomy
specimens from women at high risk for pelvic serous carcinoma.
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