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大鼠对硅酮植入物的细胞反应特征:对异物致癌作用的影响。

Characterization of cellular response to silicone implants in rats: implications for foreign-body carcinogenesis.

作者信息

James S J, Pogribna M, Miller B J, Bolon B, Muskhelishvili L

机构信息

FDA National Center for Toxicological Research, Jefferson, AR 72079, USA.

出版信息

Biomaterials. 1997 May;18(9):667-75. doi: 10.1016/s0142-9612(96)00189-5.

Abstract

Foreign-body (FB) carcinogenesis is a classic model of multistage tumour development in rodents. Previous studies have demonstrated that the physical characteristics of the implant, and not the chemical composition, are the critical determinants of tumour development. The recent controversy over silicone breast implants has raised questions regarding the potential carcinogenicity of lifetime tissue exposure to silicone products. The present study was designed to determine whether the inflammatory and fibrotic reactions associated with silicone implants are due to a non-specific foreign-body reaction or whether these responses reflect the unique chemical composition of silicone. F344 rats were implanted subcutaneously with one of three biomaterials: silicone elastomer (Group 1); impermeable cellulose acetate filters (Group 2, positive control); or porous cellulose acetate filters (Group 3, negative control). The silicone and cellulose implants of Groups 1 and 2 have been previously shown to induce fibrosarcomas in rodents, whereas the porous cellulose acetate implants of Group 3 have been shown to be non-carcinogenic. One week and two months after implantation, the pericapsular tissues were evaluated using histopathological and in situ immunohistochemical analyses. Endpoints included expression of leucocyte antigens CD4 (T helper/inducer), CD8 (T suppressor/cytotoxic) and CD11 b/c (macrophage), proliferating cell nuclear antigen (PCNA) as an indicator of proliferation, and in situ end-labelling (ISEL) of 3'OH DNA strand breaks as an indicator of DNA damage and apoptosis. The results indicated that the acute and chronic cellular responses to silicone (Group 1) were not different from impermeable cellulose filters (Group 2) of identical size and shape, suggesting that these responses were not unique to silicone. The inflammatory response to the carcinogenic cellulose and silicone implants (Groups 1 and 2) was attenuated and associated with the formation of a thick fibrotic capsule. In contrast, the porous cellulose filters (Group 3) induced a markedly different cellular response in which the inflammatory reaction was more extensive, prolonged and associated with minimal fibrosis. Within the fibrotic capsule surrounding the tumorigenic implants, but not the non-tumorigenic implants, cell proliferation and apoptotic cell death were increased and associated with persistent DNA strand breaks. Taken together, the results suggest that the micrometre-scale surface morphology of the implant determines the nature of the subsequent cellular response which may predispose to tumour development. Further, these studies serve to emphasize the critical importance of appropriate physical controls in studies designed to evaluate carcinogenic or autoimmune manifestations associated with silicone implants in order to rule out the contribution of the chronic foreign-body reaction.

摘要

异物(FB)致癌作用是啮齿动物多阶段肿瘤发展的经典模型。先前的研究表明,植入物的物理特性而非化学成分是肿瘤发展的关键决定因素。最近关于硅胶乳房植入物的争议引发了人们对终生组织暴露于硅胶产品潜在致癌性的质疑。本研究旨在确定与硅胶植入物相关的炎症和纤维化反应是由于非特异性异物反应,还是这些反应反映了硅胶独特的化学成分。将F344大鼠皮下植入三种生物材料之一:硅胶弹性体(第1组);不透性醋酸纤维素滤膜(第2组,阳性对照);或多孔醋酸纤维素滤膜(第3组,阴性对照)。第1组和第2组的硅胶和纤维素植入物先前已被证明可在啮齿动物中诱发纤维肉瘤,而第3组的多孔醋酸纤维素植入物已被证明无致癌性。植入后1周和2个月,使用组织病理学和原位免疫组化分析对包膜组织进行评估。观察指标包括白细胞抗原CD4(T辅助/诱导细胞)、CD8(T抑制/细胞毒性细胞)和CD11b/c(巨噬细胞)的表达,增殖细胞核抗原(PCNA)作为增殖指标,以及3'OH DNA链断裂的原位末端标记(ISEL)作为DNA损伤和凋亡指标。结果表明,对硅胶(第1组)的急性和慢性细胞反应与相同大小和形状的不透性纤维素滤膜(第2组)没有差异,这表明这些反应并非硅胶所特有。对致癌性纤维素和硅胶植入物(第1组和第2组)的炎症反应减弱,并与厚纤维化包膜的形成有关。相比之下,多孔醋酸纤维素滤膜(第3组)诱导出明显不同的细胞反应,其中炎症反应更广泛、持续时间更长且纤维化程度最小。在致瘤性植入物周围的纤维化包膜内,但非致瘤性植入物周围,细胞增殖和凋亡性细胞死亡增加,并与持续的DNA链断裂有关。综上所述,结果表明植入物的微米级表面形态决定了随后细胞反应的性质,这可能易导致肿瘤发展。此外,这些研究强调了在旨在评估与硅胶植入物相关的致癌或自身免疫表现的研究中适当物理对照的至关重要性,以便排除慢性异物反应的影响。

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