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Diagnostic Utility of SATB2 in Metastatic Krukenberg Tumors of the Ovary: An Immunohistochemical Study of 70 Cases With Comparison to CDX2, CK7, CK20, Chromogranin, and Synaptophysin.

SATB2在卵巢Krukenberg瘤中的诊断应用:与CDX2、CK7、CK20、CgA、SYN的免疫组化对比70例研究

Yang C,Sun L,Zhang L,Zhou L,Zhao M,Peng Y,Niu D,Li Z,Huang X,Kang Q,Jia L,Lai J,Cao D

Abstract

SATB2 is a sensitive marker for colorectal adenocarcinomas. No study has investigated its diagnostic utility in metastatic Krukenberg tumors (MKTs) of the ovary. Here we performed immunohistochemical staining SATB2 in 70 MKTs of various origins (stomach 27, colorectum 13, appendix 20 including 19 metastatic adenocarcinomas ex goblet cell carcinoids [AdexGCC] and 1 conventional poorly differentiated carcinoma with signet ring cells, breast 5, bladder 3, lung 2) to assess its diagnostic utility. We also compared SATB2 with CDX2, CK7, CK20, chromogranin, and synaptophysin in MKTs of gastric origin (MKTs-stomach), those of colorectal origin (MKTs-colorectum) and those due to appendiceal AdexGCCs (MKT-AdexGCCs) for their sensitivity and specificity to distinguish these tumors. SATB2 staining was seen in 1/27 (4%) MKTs-stomach (40% cells), 7/13 (54%) MKTs-colorectum (mean: 17% cells, median: 7%, range: 2% to 60%), and 19/19 (100%) of MKT-AdexGCCs (mean: 97% cells, median: 100%, range: 80% to 100%) (P<0.01 between any two). SATB2 staining was seen in 1/1 metastatic appendiceal poorly differentiated carcinoma with signet ring cells (5% cells), 1/3 MKTs of bladder origin (60% cells), 0/2 MKTs of pulmonary origin, and 1/5 MKTs of breast origin (10% cells). SATB2 staining was diffuse strong in MKT-AdexGCCs whereas in other MKTs it was focal and weak in the signet ring and nonsignet ring nonglandular cells and from focal weak to diffuse strong in well-formed glands. MKTs-stomach, MKTs-colorectum, and MKT-AdexGCCs showed no significant staining difference in CDX2 (100%, 100%, 100% cases, respectively; P=1.0), CK20 (96%, 100%, 100%, respectively; P=1.0), chromogranin (59%, 31%, 63%, respectively; P>0.05) or synaptophysin (59%, 63%, 84%, respectively; P>0.05) but they had significant difference in CK7 staining (93%, 8%, 42%, respectively; P<0.05). Among these 6 markers, SATB2 is the best one to distinguish MKT-AdexGCCs from MKTs-stomach (100% sensitivity, 96% specificity) and MKTs-colorectum (100% sensitivity and 100% specificity if staining more than 75% tumor cells as the cutoff). In distinguishing MKTs-stomach from MKTs-colorectum, SATB2 is not as good as CK7 which is the best marker. Our results indicate that SATB2 is a highly sensitive marker (100% sensitivity) for metastatic MKT-AdexGCCs with high specificity (100% specificity when showing strong staining in at least 75% cells) among MKTs. SATB2 is a useful marker for determining the primary sites of MKTs of the ovary.

摘要

SATB2是一个结直肠腺癌的敏感指标,目前尚无它在卵巢转移性Krukenberg瘤(MKTs)诊断中应用的研究,本研究对70例来源于不同器官的MKTs进行SATB2免疫组化染色(包括27例胃,13例结直肠,20例阑尾,其中包括19例非杯状细胞类癌的转移性腺癌和1例伴有印戒细胞的低分化癌,5例乳腺,3例膀胱,2例肺)来评估其诊断价值。我们对比了SATB2与CDX2、CK7、CK20、CgA、SYN在鉴别来自胃、结直肠、阑尾AdexGCCs的MKTs敏感性及特异性。SATB2在MKTs-胃中1/27(4%)表达(40%细胞),MKTs-结直肠中7/13(54%)表达(平均:17%细胞,中位数:7%细胞,范围:2%-60%),MKT-AdexGCCs中19/19(100%)表达(平均:97%细胞,中位数:100%,范围:80%-100%)(两两比较,P<0.01)。SATB2在转移性阑尾伴印戒细胞的低分化癌中1/1表达(60%细胞),MKTs-膀胱1/3表达(60%细胞),2例MKTs-肺中均未表达(0/2),MKTs-乳腺1/5表达(10%细胞)。SATB2在MKT-AdexGCCs中弥漫强阳,而在印戒细胞及非印戒非腺样MKTs中局灶或弱阳性,在分化好区域弥漫强阳。CDX2(分别为100%,100%,100%病例表达,P=1.0),CK20(分别为96%,100%,100%,P=1.0),CgA(分别为59%,31%,63%,P>0.05),SYN(分别为59%,63%,84%,P>0.05)在鉴别MKTs-胃,MKTs-结直肠和MKT-AdexGCCs中未见明显差异,而CK7(分别为93%,8%,42%,P<0.05)在鉴别3者上差异有统计学意义。这6个标记物中,SATB2是鉴别MKT-AdexGCCs与MKTs-胃(敏感度100%,特异度96%)、MKTs-结直肠(敏感度100%,特异度100%,cutoff值75%)的最好指标。CK7是鉴别MKTs-胃与MKTs-结直肠的最好标记物。结果提示SATB2对诊断MKT-AdexGCCs来说是一个高度敏感(敏感度100%)和特异(特异度100%,至少75%细胞强阳)的指标。SATB2在判断卵巢MKTs的来源上是一个有用的指标。

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