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用于乳腺硅胶植入物免疫毒理学评估的高效体外模型。

Efficient in vitro model for immunotoxicologic assessment of mammary silicone implants.

作者信息

Rhie J W, Han S B, Byeon J H, Ahn S T, Kim H M

机构信息

Department of Plastic Surgery, Catholic University Medical College, Youngdungpogu, Taejon City, Korea.

出版信息

Plast Reconstr Surg. 1998 Jul;102(1):73-7. doi: 10.1097/00006534-199807000-00011.

Abstract

In clinical and experimental studies, silicone gel has been assumed to cause immune alterations that may be related to macrophage activation of silicone implants. However, it has not been proven that the immunotoxicities are caused by the direct contact of macrophages and silicone gel because there has not been an adequate experimental model. In the present study, silicone gel was loaded directly onto Petri dishes and was distributed uniformly to the bottom by centrifugation. Peritoneal macrophages and splenic lymphocytes were cultured either on the silicone-coated plates or on the conventional, normal plates, and their functions were compared with each other. The experiments were repeated three times. The cytotoxic activities of peritoneal macrophages on cancer cells were markedly augmented by cultivation on silicone gel, and the primary T-dependent immunoglobulin M response in which macrophages participated as antigen presenting cells was also enhanced by incubation on silicone gel. However, macrophage-unrelated functions mediated by B and T lymphocytes were not affected by the silicone gel treatment. It was proven that the direct contact of macrophages with silicone gel was a primary cause of acute immune activation that was related to foreign body reaction. In addition, the present in vitro model exhibited similar silicone-induced immunotoxicities in previous animal and clinical studies.

摘要

在临床和实验研究中,硅凝胶被认为会引起免疫改变,这可能与硅植入物的巨噬细胞活化有关。然而,尚未证实免疫毒性是由巨噬细胞与硅凝胶的直接接触所致,因为缺乏适当的实验模型。在本研究中,将硅凝胶直接加载到培养皿上,并通过离心使其均匀分布于底部。将腹腔巨噬细胞和脾淋巴细胞分别培养在涂有硅凝胶的平板或传统的正常平板上,并比较它们的功能。实验重复进行了三次。在硅凝胶上培养可显著增强腹腔巨噬细胞对癌细胞的细胞毒活性,并且巨噬细胞作为抗原呈递细胞参与的初次T细胞依赖性免疫球蛋白M反应在硅凝胶上孵育时也得到增强。然而,由B淋巴细胞和T淋巴细胞介导的与巨噬细胞无关的功能不受硅凝胶处理的影响。已证实巨噬细胞与硅凝胶的直接接触是与异物反应相关的急性免疫激活的主要原因。此外,本体外模型在先前的动物和临床研究中表现出类似的硅诱导的免疫毒性。

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