Kim Y S, Kim K H, Choi J A, Lee J H, Kim H K, Won N H, Kim I
Department of Pathology, College of Medicine, Korea University, Gojan-Dong, Ansan, Korea.
Arch Pathol Lab Med. 2000 May;124(5):687-93. doi: 10.5858/2000-124-0687-FACLAF.
Fas ligand (FasL, CD95L) is a type II transmembrane protein of the tumor necrosis factor family that induces cells to send an apoptotic signal to cells expressing Fas (CD95, APO-1). It has been shown that cancers have a dysregulated expression of Fas and FasL system, conferring a survival advantage. It is important to understand FasL and Fas expression in tumors, because the growth of cancer might be controlled by Fas-mediated apoptosis.
The expressions of FasL and Fas were studied by immunohistochemical analyses in 51 cases of renal cell carcinomas and the adjacent normal renal tissues, respectively. In addition, their expressions were compared with prognostic factors, such as tumor size, nuclear grade, TNM stage, and histologic types.
In nonneoplastic renal tissues, FasL was expressed in all nephron segments, whereas Fas also expressed in all tubules, except for glomeruli. In renal cell carcinomas, FasL protein was detected in 50 (98.0%) of 51 cases, whereas Fas expressed in 38 (74.5%) of 51 cases. In fact, the immunostaining of Fas was less intense than that in the adjacent normal segments of all cases. The staining pattern showing both high expression of FasL and low expression of Fas was found in 36 (70.6%) (P = .04) of 51 cases, most of which were Fuhrman grade 2 or 3 tumors. However, the expression pattern did not correlate statistically with the tumor size, histologic type, or clinical stage. On the other hand, most grade 4 tumors displayed high expression of both FasL and Fas (P<.001).
These data indicate that high expression of FasL and low expression of Fas protein in renal cell carcinomas may play a role in evading surveillance of the immune system. In addition, the FasL and Fas expressions appear to have a therapeutic implication for high-grade tumors rather than a prognostic one.
Fas配体(FasL,CD95L)是肿瘤坏死因子家族的一种II型跨膜蛋白,可诱导细胞向表达Fas(CD95,APO-1)的细胞发送凋亡信号。研究表明,癌症中Fas和FasL系统表达失调,从而赋予其生存优势。了解肿瘤中FasL和Fas的表达很重要,因为癌症的生长可能受Fas介导的凋亡控制。
分别采用免疫组化分析研究51例肾细胞癌及其相邻正常肾组织中FasL和Fas的表达。此外,将它们的表达与肿瘤大小、核分级、TNM分期和组织学类型等预后因素进行比较。
在非肿瘤性肾组织中,FasL在所有肾单位节段均有表达,而Fas除肾小球外,在所有肾小管中也有表达。在肾细胞癌中,51例中有50例(98.0%)检测到FasL蛋白,而51例中有38例(74.5%)表达Fas。事实上,所有病例中Fas的免疫染色强度均低于相邻正常节段。51例中有36例(70.6%)出现FasL高表达和Fas低表达的染色模式(P = 0.04),其中大多数为Fuhrman 2级或3级肿瘤。然而,这种表达模式与肿瘤大小、组织学类型或临床分期无统计学相关性。另一方面,大多数4级肿瘤同时显示FasL和Fas高表达(P<0.001)。
这些数据表明,肾细胞癌中FasL高表达和Fas蛋白低表达可能在逃避免疫系统监测中起作用。此外,FasL和Fas的表达似乎对高级别肿瘤具有治疗意义,而非预后意义。