有机硅凝胶促进新西兰黑鼠自身免疫性疾病的发展,但在BALB/cAnPt小鼠中不能诱导

Ann H. McDonald , Michelle Schneider , Lynn Gudenkauf , James R. Sanger , Kimberly Weir
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引用次数: 26

摘要

轶事证据表明硅胶乳房植入物与女性自身免疫性结缔组织疾病的发展有关。为了研究硅胶是否能够直接诱导和/或增强自身免疫性疾病的发展,将雌性BALB/cAnPt (BALB/c)和新西兰黑(NZB)小鼠皮下注射硅胶、pristane(一种可引起BALB/c和NZB小鼠浆细胞瘤的非代谢物质)或生理盐水,并监测肾小球肾炎的发展和自身抗体的产生。在12个月大时,小鼠自发地产生自身抗体和自身免疫性溶血性贫血,而不是BALB/c。在10个月的时间里,每两周一次的蛋白尿筛查显示,多次注射硅胶或普里斯坦的NZB小鼠尿蛋白增加。相比之下,同样处理的BALB/c小鼠尿蛋白未受影响。虽然硅胶对NZB小鼠血清抗红细胞抗体滴度没有影响,但红细胞压积明显降低。此外,硅胶不仅增加了IgM抗I型胶原抗体的浓度,而且使HEp-2细胞血清自身抗体的免疫荧光染色模式发生偏斜。相比之下,硅凝胶不能诱导BALB/c小鼠产生抗红细胞或抗核抗体,仅诱导抗I型胶原抗体IgG轻微增加。这些结果表明,硅凝胶在自身免疫性NZB小鼠中可加剧自身免疫性疾病的发展,但在正常BALB/c小鼠中不能诱导疾病。这与几项流行病学研究一致,这些研究未能证明隆胸女性自身免疫性疾病的发病率增加。然而,由于硅凝胶能够加剧NZB小鼠的自身免疫性疾病,它可能在一小部分遗传上易患此类疾病的女性的自身免疫性疾病发展中发挥类似的作用。
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Silicone Gel Enhances the Development of Autoimmune Disease in New Zealand Black Mice but Fails To Induce It in BALB/cAnPt Mice

Anecdotal evidence links silicone gel breast implants with the development of autoimmune connective tissue disease in women. To investigate whether silicone gel is capable of directly inducing and/or enhancing the development of autoimmune disease, female BALB/cAnPt (BALB/c) and New Zealand Black (NZB) mice were injected subcutaneously with silicone gel, pristane, a nonmetabolizable substance that can cause plasmacytomas in BALB/c and NZB mice, or saline and monitored for the development of glomerulonephritis and autoantibody production. NZB, but not BALB/c, mice spontaneously develop autoantibodies and an autoimmune hemolytic anemia by 12 months of age. Over a period of 10 months, biweekly screening for proteinuria revealed increases in urinary protein in NZB mice that received multiple injections of either silicone gel or pristane. In contrast, urinary protein was unaffected in identically treated BALB/c mice. Although, silicone gel had no effect on serum titers of anti-erythrocyte antibodies in NZB mice, the hematocrits were significantly decreased. Moreover, silicone gel both increased the concentration of IgM anti-type I collagen antibodies and skewed the immunofluorescent staining pattern of serum autoantibodies on HEp-2 cells. In contrast, silicone gel failed to induce the production of anti-erythrocyte or antinuclear antibodies in BALB/c mice and induced only slight increases in IgG anti-type I collagen antibodies. These results suggest that silicone gel can exacerbate the development of autoimmune disease in autoimmune NZB mice, but fails to induce disease in normal BALB/c mice. This is consistent with several epidemiological studies failing to demonstrate an increase in the incidence of autoimmune disease in women with breast implants. However, because silicone gel was able to exacerbate autoimmune disease in NZB mice, it may play a similar role in the development of autoimmune disease in a small percentage of women who are genetically susceptible to such diseases.

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