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1 clusion cysts to a conventional (high-grade) serous carcinoma.
2 53 allele occurs early in the development of serous carcinoma.
3 rotransposition events in high-grade ovarian serous carcinoma.
4 shows prognostic significance for high-grade serous carcinoma.
5 tions for mucinous, clear-cell, or low-grade serous carcinoma.
6 cer, including the highly aggressive ovarian serous carcinoma.
7 way activation have been reported in ovarian serous carcinoma.
8 greater GC UNC-45 expression than low-stage serous carcinoma.
9 s to noninvasive and invasive micropapillary serous carcinomas.
10 tage serous BOTs and later developed grade 1 serous carcinomas.
11 hways through profiling of normal FTSECs and serous carcinomas.
12 type II OvCAs, most of which are high-grade serous carcinomas.
13 er was significantly higher in HG than in LG serous carcinomas.
14 vely, in independent 47 affinity-purified HG serous carcinomas.
15 p13.12 in 6 of 31 (19.5%) ovarian high-grade serous carcinomas.
16 oved disease-specific survival in high-grade serous carcinoma (0.71, 0.55-0.91; p=0.0080), but weak P
17 n cancer were included: 1742 with high-grade serous carcinoma, 110 with low-grade serous carcinoma, 2
19 h-grade serous carcinoma, 110 with low-grade serous carcinoma, 207 with mucinous carcinoma, 484 with
20 s borderline tumors, but among the low-grade serous carcinomas (39 stage III, 2 stage II, and 2 stage
21 R-2 expression and amplification was seen in serous carcinoma (43% and 29%), while grade 1 endometrio
23 ive histological subtypes (uterine papillary serous carcinoma and clear cell carcinoma, UPSC/CCC) by
24 the majority representing uterine papillary serous carcinoma and mixed malignant mesodermal tumor.
25 a demonstrate that MI is uncommon in uterine serous carcinoma and support that different pathogenetic
27 ian tumors (BOT) can progress into low-grade serous carcinomas and have relatively indolent clinical
28 except frequent p53 mutations in high-grade serous carcinomas and malignant mixed mesodermal tumors
29 fimbria as a field of origin for high-grade serous carcinomas and present a binary model of ovarian
30 -1 is significantly overexpressed in ovarian serous carcinomas and several other types of carcinomas.
31 arian neoplastic lesions, especially uterine serous carcinomas, and suggest that mutation of PPP2R1A
32 , and seromucinous carcinomas; ii) low-grade serous carcinomas; and iii) mucinous carcinomas and mali
33 ate that the precursor of ovarian high-grade serous carcinoma appears to develop from an occult intra
35 indings, suggests that aggressive, low-grade serous carcinomas are more likely derived from serous bo
37 ors (SBTs), putative precursors of low-grade serous carcinomas, are among the few human neoplasms wit
38 of the PI3K pathway, we show that high-grade serous carcinomas arise from the fallopian tube in mice.
39 found that advanced-stage, low-grade ovarian serous carcinomas both with and without adjacent serous
40 r cell carcinoma (Arid1a, Pik3ca), low-grade serous carcinoma (Braf), endometrioid (Ctnnb1), or mucin
41 en observed at high frequency in endometrial serous carcinomas but at low frequency in ovarian clear
43 face epithelial cell line and in a low-grade serous carcinoma cell line that expressed undetectable l
44 Most notable of these tumours are papillary serous carcinomas, clear-cell carcinomas, carcinosarcoma
47 against i.p. chemotherapy-resistant uterine serous carcinoma-derived xenografts compared with free E
48 hat Nrf2 was highly expressed in endometrial serous carcinoma (ESC), whereas complex hyperplasia and
51 ated endometrioid, clear cell, and low-grade serous carcinomas from high-grade serous and mucinous ca
54 common subtype of ovarian cancer, high-grade serous carcinoma, has sparked a major effort within the
56 g evidence indicates that ovarian high-grade serous carcinoma (HGSC) originates from fallopian tube s
57 lantable murine models of ovarian high grade serous carcinoma (HGSC) remain an important research too
59 lantable murine models of ovarian high-grade serous carcinoma (HGSC) with regard to mutations in the
60 ocus has been detected in ovarian high-grade serous carcinoma (HGSC), the most common and malignant t
61 cantly increased risk for ovarian high-grade serous carcinoma (HGSC; 3.8% cases vs. 0.2% controls).
62 al fallopian tube among all cases.High-grade serous carcinomas (HGSCs) are associated with precursor
65 cent studies suggest that >50% of high-grade serous carcinomas involving the ovary likely arise from
66 in the MI frequency between endometrioid and serous carcinoma is statistically significant (P = 0.003
67 common surface epithelial tumors, low-grade serous carcinoma is the prototypic type I tumor and high
69 cular pathogenesis of fallopian tube-derived serous carcinomas is poorly understood and there are few
71 profiled the DNA methylomes of 12 low-grade serous carcinomas (LGSCs), 19 SBOTs, and 16 benign serou
72 carcinoma (log-rank p<0.0001) and high-grade serous carcinoma (log-rank p=0.0006), and ER expression
74 e tumors (SBTs), non-invasive micropapillary serous carcinomas (MPSCs), and invasive micropapillary s
76 rous borderline tumors (n = 30) or low-grade serous carcinomas (n = 43) but were found in 73% of high
84 loss patterns on chromosome 17 to papillary serous carcinoma of the peritoneum (PSCP) which is histo
85 h a platinum- and taxane-resistant papillary serous carcinoma of the peritoneum experienced a partial
89 re common type of ovarian cancer, high-grade serous carcinoma, ovarian CCC is often resistant to plat
90 ation of chemotherapy in ovarian and uterine serous carcinoma patients by biodegradable nanoparticles
91 cated that full-length ALK expression in two serous carcinoma patients is consistent with ALK gene co
93 important role early in the pathogenesis of serous carcinoma, possibly accounting for its aggressive
95 helial ovarian carcinoma (EOC) or peritoneal serous carcinoma (PSC) who had experienced disease progr
98 r involves a genetically unstable high-grade serous carcinoma that metastasizes rapidly (type II).
99 e composed, for the most part, of high-grade serous carcinomas that can be further subdivided into mo
101 xpression was frequently detected in ovarian serous carcinomas, the most common and lethal type of ov
102 number alterations in 31 high-grade ovarian serous carcinomas, the most lethal gynecologic neoplasti
103 ll as a cell of origin for high-grade pelvic serous carcinomas, the need to develop tools and model s
104 cally resembled the in situ precursor of TII serous carcinomas; these lesions have not been observed
106 among patients with stage II to IV low-grade serous carcinoma treated with primary surgery followed b
112 serous BOTs and subsequent grade 1 papillary serous carcinomas was microdissected and retrieved using
114 enome-wide homozygous deletion profile in HG serous carcinomas, which can serve as a molecular founda
115 BRAF mutations in advanced-stage, low-grade serous carcinomas, which contrasts with previous finding
116 cinomas (MPSCs), and invasive micropapillary serous carcinomas, which represent a morphological conti
117 nclusion Women with stage II to IV low-grade serous carcinoma who received HMT after primary treatmen
118 trioid adenocarcinomas and uterine papillary serous carcinomas, ZEB1 could be expressed in the epithe
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