Wang M-H, Grossmann M E, Young C Y F
Department of Urology and Biochemistry/Molecular Biology, Mayo Graduate School, Mayo Clinic/Foundation, Rochester, MN 55905, USA.
Br J Cancer. 2004 Feb 23;90(4):926-31. doi: 10.1038/sj.bjc.6601583.
Although heat-shock protein 70 (Hsp70) has been considered an intracellular protein, we report that Hsp70 is secreted under normal cell culture conditions by human prostate cell lines, LAPC-4, PC-3, CWR-22, RWPE-1 and -2, LNCaP, and TRAMP (transgenic adenocarcinoma mouse prostate)-C2. We found that the secretion can be enhanced by transfection with cDNA encoding for Hsp70. To verify that the Hsp70 detected in the supernatant was not secondary to cell leakage, C2 cells were cotransfected with cytoplasmic Renilla luciferase as a reporter. High levels of activities were noted in the cell extracts, while no enzyme activities were detected in the supernatants. To verify that forced oversecretion of Hsp70 could protect against tumour growth, mice were injected with C2 cells transfected with an Hsp70 DNA construct and challenged with live tumour cells. Mice injected with cells transfected with the Hsp70 DNA construct demonstrated a significantly decreased rate of tumour growth compared to those injected with empty vector. In addition, a difference in survival rate as defined by a surrogate end point was noted between the two groups. In a second experiment, we developed a cell line that stably overexpressed Hsp70. Mice injected with these cells also demonstrated a significant decrease in tumour growth and significantly increased survival.
尽管热休克蛋白70(Hsp70)一直被认为是一种细胞内蛋白,但我们报告称,在正常细胞培养条件下,人前列腺细胞系LAPC-4、PC-3、CWR-22、RWPE-1和-2、LNCaP以及TRAMP(转基因腺癌小鼠前列腺)-C2会分泌Hsp70。我们发现,通过转染编码Hsp70的cDNA可以增强这种分泌。为了验证在上清液中检测到的Hsp70并非细胞渗漏所致,将C2细胞与作为报告基因的细胞质海肾荧光素酶共转染。在细胞提取物中检测到高水平的活性,而上清液中未检测到酶活性。为了验证Hsp70的强制过度分泌是否能预防肿瘤生长,给小鼠注射用Hsp70 DNA构建体转染的C2细胞,并接种活肿瘤细胞。与注射空载体的小鼠相比,注射用Hsp70 DNA构建体转染的细胞的小鼠肿瘤生长速率显著降低。此外,两组之间在由替代终点定义的存活率方面存在差异。在第二项实验中,我们构建了一个稳定过表达Hsp70的细胞系。注射这些细胞的小鼠肿瘤生长也显著降低,存活率显著提高。
