Biphasic papillary and lobular breast carcinoma with PIK3CA and IDH1 mutations.

Daphne Ang, Amanda M VanSandt, Carol Beadling, Andrea Warrick, Robert B West, Christopher L Corless, Megan L Troxell
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引用次数: 16

Abstract

Morphologic "special types" of breast carcinomas have been recognized for many years, and their molecular and genetic properties have not been specifically studied until recently. Lobular carcinoma lacks functional E-cadherin expression but shares molecular similarities with low-grade invasive ductal carcinomas. Papillary carcinoma is relatively rare, and molecular features are just being elucidated. We report a case of concurrent invasive lobular and papillary carcinoma, the latter with extensive nodal involvement. Multiplex screening for activating point mutations identified different point mutations in the distinct morphologic components: lobular PIK3CA H1047R, papillary; PIK3CA Q546P, and IDH1 R132H. These molecular data favor coincidental "collision tumors" over clonal evolution. The IDH1 R132H point mutation is common in gliomas and acute myelogenous leukemia, but this has not been previously reported in breast carcinoma. The characterization of activating point mutations in morphologic special types of breast carcinoma may suggest avenues amenable to targeted therapy.

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PIK3CA和IDH1突变的双期乳头状和小叶性乳腺癌。
形态学上的“特殊类型”乳腺癌已被认识多年,直到最近才对其分子和遗传特性进行专门研究。小叶癌缺乏功能性E-cadherin表达,但与低级别浸润性导管癌具有分子相似性。乳头状癌相对罕见,其分子特征刚刚被阐明。我们报告一例同时浸润的小叶和乳头状癌,后者有广泛的淋巴结累及。激活点突变的多重筛选鉴定出不同形态成分的不同点突变:小叶PIK3CA H1047R、乳头状;PIK3CA Q546P, IDH1 R132H。这些分子数据支持巧合的“碰撞肿瘤”而不是克隆进化。IDH1 R132H点突变在胶质瘤和急性髓性白血病中很常见,但在乳腺癌中尚未报道。形态学特殊类型乳腺癌中活化点突变的特征可能为靶向治疗提供途径。
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期刊介绍: Diagnostic Molecular Pathology focuses on providing clinical and academic pathologists with coverage of the latest molecular technologies, timely reviews of established techniques, and papers on the applications of these methods to all aspects of surgical pathology and laboratory medicine. It publishes original, peer-reviewed contributions on molecular probes for diagnosis, such as tumor suppressor genes, oncogenes, the polymerase chain reaction (PCR), and in situ hybridization. Articles demonstrate how these highly sensitive techniques can be applied for more accurate diagnosis.
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