Institute of Cytology of Russian Academy of Sciences, Tikhoretsky Ave. 4, St. Petersburg, Russia, 194064.
St.Petersburg Nuclear Physics Institute Named By B.P. Konstantinov of National Research Centre «Kurchatov Institute», Orlova roshcha 1, Gatchina, Russia, 188300.
Sci Rep. 2021 Oct 29;11(1):21314. doi: 10.1038/s41598-021-00734-4.
The release of Hsp70 chaperone from tumor cells is found to trigger the full-scale anti-cancer immune response. Such release and the proper immune reaction can be induced by the delivery of recombinant Hsp70 to a tumor and we sought to explore how the endogenous Hsp70 can be transported to extracellular space leading to the burst of anti-cancer activity. Hsp70 transport mechanisms were studied by analyzing its intracellular tracks with Rab proteins as well as by using specific inhibitors of membrane domains. To study Hsp70 forms released from cells we employed the assay consisting of two affinity chromatography methods. Hsp70 content in culture medium and extracellular vesicles (EVs) was measured with the aid of ELISA. The properties and composition of EVs were assessed using nanoparticle tracking analysis and immunoblotting. The activity of immune cells was studied using an assay of cytotoxic lymphocytes, and for in vivo studies we employed methods of affinity separation of lymphocyte fractions. Analyzing B16 melanoma cells treated with recombinant Hsp70 we found that the chaperone triggered extracellular transport of its endogenous analog in soluble and enclosed in EVs forms; both species efficiently penetrated adjacent cells and this secondary transport was corroborated with the strong increase of Natural Killer (NK) cell toxicity towards melanoma. When B16 and CT-26 colon cancer cells before their injection in animals were treated with Hsp70-enriched EVs, a powerful anti-cancer effect was observed as shown by a two-fold reduction in tumor growth rate and elevation of life span. We found that the immunomodulatory effect was due to the enhancement of the CD8-positive response and anti-tumor cytokine accumulation; supporting this there was no delay in CT-26 tumor growth when Hsp70-enriched EVs were grafted in nude mice. Importantly, pre-treatment of B16 cells with Hsp70-bearing EVs resulted in a decline of arginase-1-positive macrophages, showing no generation of tumor-associated macrophages. In conclusion, Hsp70-containing EVs generated by specifically treated cancer cells give a full-scale and effective pattern of anti-tumor immune responses.
从肿瘤细胞中释放热休克蛋白 70(Hsp70)被发现会引发全面的抗癌免疫反应。这种释放和适当的免疫反应可以通过将重组 Hsp70 递送到肿瘤中来诱导,我们试图探索内源性 Hsp70 如何被运输到细胞外空间,从而导致抗癌活性的爆发。通过分析其与 Rab 蛋白的细胞内轨迹以及使用膜结构域的特定抑制剂,研究了 Hsp70 的运输机制。为了研究从细胞中释放的 Hsp70 形式,我们采用了由两种亲和层析方法组成的测定法。使用 ELISA 测量培养基和细胞外囊泡(EVs)中的 Hsp70 含量。使用纳米颗粒跟踪分析和免疫印迹评估 EVs 的特性和组成。使用细胞毒性淋巴细胞测定法研究免疫细胞的活性,并且对于体内研究,我们采用了亲和分离淋巴细胞分数的方法。分析用重组 Hsp70 处理的 B16 黑色素瘤细胞,我们发现该伴侣蛋白触发了其内源性类似物以可溶性和包裹在 EVs 形式的细胞外运输;两种物质都有效地穿透相邻细胞,并且这种二次运输与 NK 细胞对黑色素瘤的毒性的强烈增加相吻合。当在注射动物之前用 Hsp70 富集的 EVs 处理 B16 和 CT-26 结肠癌细胞时,观察到强大的抗癌作用,表现为肿瘤生长速度降低了两倍,寿命延长了。我们发现,免疫调节作用是由于增强了 CD8 阳性反应和抗肿瘤细胞因子的积累所致;支持这一点的是,在裸鼠中移植富含 Hsp70 的 EVs 时,CT-26 肿瘤的生长没有延迟。重要的是,用 Hsp70 携带的 EVs 预处理 B16 细胞会导致精氨酸酶 1 阳性巨噬细胞的减少,表明不会产生肿瘤相关巨噬细胞。总之,经专门处理的癌细胞产生的含有 Hsp70 的 EVs 会引发全面有效的抗肿瘤免疫反应模式。
