TIM3(+) breast cancer cells license immune evasion during micrometastasis outbreak.

TIM3(+)乳腺癌细胞在微转移爆发期间可逃避免疫攻击

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作者:Rozalén Catalina, Sangrador Irene, Avalle Silvia, Blasco-Benito Sandra, Tzortzi Panagiota, Sanz-Flores María, Palomeque José Ángel, Torren-Duran Pau, Dalmau Mariona, Brunel Helena, Coll-Manzano Albert, Pérez-Núñez Iván, Martos Tamara, Servitja Sonia, Pérez-Buira Sandra, Chacón José Ignacio, Guerrero-Zotano Ángel, Martínez de Dueñas Eduardo, Guillén Yolanda, Comerma Laura, Bermejo Begoña, Bigas Anna, Casanova-Acebes María, Alemany Anna, Rojo Federico, Albanell Joan, Celià-Terrassa Toni
期刊:Cancer Cell影响因子:44.500
时间:2025起止号:2025 Aug 11; 43(8):1549-1567
doi:10.1016/j.ccell.2025.06.015研究方向: 细胞生物学
疾病类型: 乳腺癌
In metastasis, the dynamics of tumor-immune interactions during micrometastasis remain unclear. Identifying the vulnerabilities of micrometastases before outbreaking into macrometastases can reveal therapeutic opportunities for metastasis. Here, we report a function of T cell immunoglobulin and mucin domain 3 (TIM3) in tumor cells during micrometastasis using breast cancer (BC) metastasis mouse models. TIM3 is highly upregulated in micrometastases, promoting survival, stemness, and immune escape. TIM3(+) tumor cells are specifically selected during early seeding of micrometastasis. Mechanistically, TIM3 increases β-catenin/interleukin-1β (IL-1β) signaling, leading to stemness and immune-evasion by inducing immunosuppressive γδ T cells and reducing CD8 T cells during micrometastasis. Clinical data confirm increased TIM3(+) tumor cells in BC metastasis and TIM3(+) tumor cells as a biomarker of poor outcome in BC patients. (Neo)adjuvant TIM3 blockade reduces the metastatic seeding and incidence in preclinical models. These findings unveil a specific mechanism of micrometastasis immune-evasion and the potential use of TIM3 blockade for subclinical metastasis.

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