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免疫组织化学在鉴别原发性与继发性乳腺外佩吉特病中的作用。

The role of immunohistochemistry in discriminating primary from secondary extramammary Paget disease.

作者信息

Perrotto John, Abbott Jared J, Ceilley Roger I, Ahmed Iftikhar

机构信息

Dermatology PC, West Des Moines, IA, USA.

出版信息

Am J Dermatopathol. 2010 Apr;32(2):137-43. doi: 10.1097/DAD.0b013e3181b71481.

Abstract

BACKGROUND

Extramammary Paget disease (EMPD) is categorized into 2 groups: primary EMPD or EMPD secondary to underlying malignancy. Primary EMPD has a better prognosis, and the ability to distinguish between the 2 subsets has clinical relevance. Recent studies have suggested that immunostains, including cytokeratin (CK) 7, CK20, and BRST-2, distinguish between the 2 groups. We analyzed a large series of EMPD with an expanded immunohistochemical panel to assess its value in distinguishing primary from secondary disease.

DESIGN

Formalin-fixed, paraffin-embedded sections of 98 EMPD specimens from 61 patients (45 primary and 16 secondary) were immunostained with CK7, CK20, HER-2/neu, BRST-2, CDX2, androgen receptor (AR), and cyclin D1. The study included 44 women and 17 men (median age: 73 years). Median follow-up time was 47 months.

RESULTS

All EMPD specimens were vibrantly positive for CK7. The frequency of positivity for all EMPD samples was CK20 (28%), BRST-2 (40%), HER-2/neu (64%), CDX2 (10%), AR (16%), and cyclin D1 (76%). For primary EMPD, the frequency of positivity was CK20 (22%), BRST-2 (48%), HER-2/neu (65%), CDX2 (2%), AR (21%), and cyclin D1 (84%). For secondary EMPD, the frequency of positivity was CK20 (50%), BRST-2 (25%), HER-2/neu (60%), CDX2 (33%), AR (0%), and cyclin D1 (53%). Notably, all 6 of 7 cases of EMPD secondary to an anorectal adenocarcinoma tested were HER-2/neu negative and 5 of those 6 cases (80%) were CDX2 positive.

CONCLUSIONS

The role of CK7, CK20, and BRST-2 in distinguishing primary and secondary EMPD is limited because CK20 and BRST-2 were positive in large subsets of both groups. An expanded immunohistochemical panel, including HER-2/neu and CDX2, may be useful in discriminating primary EMPD from EMPD secondary to anorectal adenocarcinoma but fails to distinguish primary EMPD from EMPD secondary to urothelial or prostatic malignancy. The consistent overexpression of HER-2/neu in primary EMPD suggests a role for trastuzumab therapy in patients with recurrent disease.

摘要

背景

乳腺外佩吉特病(EMPD)分为两组:原发性EMPD或继发于潜在恶性肿瘤的EMPD。原发性EMPD预后较好,区分这两个亚组的能力具有临床意义。最近的研究表明,包括细胞角蛋白(CK)7、CK20和BRST-2在内的免疫染色可区分这两组。我们分析了一大系列EMPD病例,并采用扩展的免疫组织化学检测组合来评估其在区分原发性疾病和继发性疾病方面的价值。

设计

对61例患者(45例原发性和16例继发性)的98份EMPD标本进行福尔马林固定、石蜡包埋,然后用CK7、CK20、HER-2/neu、BRST-2、CDX2、雄激素受体(AR)和细胞周期蛋白D1进行免疫染色。该研究纳入了44名女性和17名男性(中位年龄:73岁)。中位随访时间为47个月。

结果

所有EMPD标本的CK7均呈强阳性。所有EMPD样本的阳性频率分别为:CK20(28%)、BRST-2(40%)、HER-2/neu(64%)、CDX2(10%)、AR(16%)和细胞周期蛋白D1(76%)。对于原发性EMPD,阳性频率分别为:CK20(22%)、BRST-2(48%)、HER-2/neu(65%)、CDX2(2%)、AR(21%)和细胞周期蛋白D1(84%)。对于继发性EMPD,阳性频率分别为:CK20(50%)、BRST-2(25%)、HER-2/neu(60%)、CDX2(33%)、AR(0%)和细胞周期蛋白D1(53%)。值得注意的是,所检测的7例继发于直肠腺癌的EMPD病例中有6例HER-2/neu呈阴性,其中5例(80%)CDX2呈阳性。

结论

CK7、CK20和BRST-2在区分原发性和继发性EMPD方面的作用有限,因为CK20和BRST-2在两组的大部分病例中均呈阳性。包括HER-2/neu和CDX2在内的扩展免疫组织化学检测组合可能有助于鉴别原发性EMPD和继发于直肠腺癌的EMPD,但无法区分原发性EMPD和继发于尿路上皮或前列腺恶性肿瘤的EMPD。原发性EMPD中HER-2/neu的持续过表达提示曲妥珠单抗治疗对复发患者可能有效。

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