Division of Medical Oncology, Department of Medicine.
Department of Biochemistry and Molecular Genetics.
JCI Insight. 2020 Feb 27;5(4):130751. doi: 10.1172/jci.insight.130751.
Small primary breast cancers can show surprisingly high potential for metastasis. Clinical decision-making for tumor aggressiveness, including molecular profiling, relies primarily on analysis of the cancer cells. Here we show that this analysis is insufficient - that the stromal microenvironment of the primary tumor plays a key role in tumor cell dissemination and implantation at distant sites. We previously described 2 cancer-associated fibroblasts (CAFs) that either express (CD146+) or lack (CD146-) CD146 (official symbol MCAM, alias MUC18). We now find that when mixed with human breast cancer cells, each fibroblast subtype determines the fate of cancer cells: CD146- fibroblasts promoted increased metastasis compared with CD146+ fibroblasts. Potentially novel quantitative and qualitative proteomic analyses showed that CD146+ CAFs produced an environment rich in basement membrane proteins, while CD146- CAFs exhibited increases in fibronectin 1, lysyl oxidase, and tenascin C, all overexpressed in aggressive disease. We also show clinically that CD146- CAFs predicted for likelihood of lymph node involvement even in small primary tumors (<5 cm). Clearly small tumors enriched for CD146- CAFs require aggressive treatments.
小型原发性乳腺癌可能具有令人惊讶的高转移潜力。肿瘤侵袭性的临床决策,包括分子分析,主要依赖于癌细胞的分析。在这里,我们表明这种分析是不充分的-原发性肿瘤的基质微环境在肿瘤细胞在远处的扩散和植入中起着关键作用。我们之前描述了 2 种与癌症相关的成纤维细胞(CAF),它们要么表达(CD146+)要么缺乏(CD146-)CD146(官方符号 MCAM,别名 MUC18)。我们现在发现,当与人类乳腺癌细胞混合时,每种成纤维细胞亚型决定了癌细胞的命运:与 CD146+成纤维细胞相比,CD146-成纤维细胞促进了转移的增加。潜在的新型定量和定性蛋白质组学分析表明,CD146+CAF 产生了富含基底膜蛋白的环境,而 CD146-CAF 则增加了纤维连接蛋白 1、赖氨酰氧化酶和腱蛋白 C 的表达,这些在侵袭性疾病中均过度表达。我们还在临床上表明,即使在小的原发性肿瘤(<5cm)中,CD146-CAF 也预示着淋巴结受累的可能性。显然,富含 CD146-CAF 的小肿瘤需要积极的治疗。
