Albisser A M, McAdam K P, Perlman K, Carson S, Bahoric A, Williamson J R
Diabetes. 1983 Dec;32(12):1092-101. doi: 10.2337/diab.32.12.1092.
Highly purified regular porcine insulin was given by portable insulin pumps through indwelling vena caval catheters to 17 (13 normal, and 4 pancreatectomized) dogs initially weighing 15 +/- 2 kg at rates ranging from 2 to 10 mU/min (total 17-250 mg) over time periods ranging from 37 to 252 days. During the course of the study, many of the animals lost weight and became anemic. Since these conditions persisted and weight loss progressed even after cessation of insulin infusion, as many of the dogs as possible (15 of 17) were autopsied for microscopic studies. Large amounts of amyloid were demonstrated in the liver, kidney, spleen, and/or pancreas in 55% (6/11) of normal, and in 75% (3/4) of pancreatectomized dogs. The amyloid deposits were Congo red positive, exhibited classical apple green fluorescence under polarized light, and possessed the characteristic ultrastructural features of amyloid. Massive deposits of amyloid were observed in animals receiving as little as 17 mg of insulin over a time span of 52 days. In those animals with hepatic amyloid, marked hepatomegaly was present (i.e., 1200 +/- 250, X +/- SD, versus 300 +/- 25 g for normal animals) and preterminal serum alkaline phosphatase levels were markedly elevated (434 +/- 285 versus 30 +/- 14 IU/L for animals without hepatic amyloid). The magnitude of the hepatic amyloid deposits precludes the possibility that they represent insulin aggregates or insulin-derived products per se. No evidence of amyloid was present in any of the tissue biopsy specimens obtained prior to insulin infusion. Moreover, the possibility that this represents an immune response to the injected porcine insulin has to be viewed in light of the fact that the amino acid sequences of dog and porcine insulins are identical. It is of particular interest that the affinity of the amyloid deposits for Congo red stain was totally abolished by prior permanganate treatment, suggesting that the amyloid was derived from serum amyloid A protein rather than from immunoglobulin light chains or insulin aggregates per se. Further evidence that the protein was of the AA-type came from the initial biochemical characterization. Gel filtration on Sephadex G100 in 6 M guanidine hydrochloride identified two small molecular weight peaks of about 13,000 and 25,000 daltons, both of which inhibited the radioimmunoassay for human AA protein.(ABSTRACT TRUNCATED AT 400 WORDS)
通过便携式胰岛素泵经留置的腔静脉导管,向17只(13只正常犬和4只胰腺切除犬)初始体重为15±2千克的犬输注高度纯化的常规猪胰岛素,输注速率为2至10毫单位/分钟(总量为17 - 250毫克),持续时间为37至252天。在研究过程中,许多动物体重减轻并出现贫血。由于这些情况持续存在,甚至在停止胰岛素输注后体重仍继续下降,因此尽可能多地对犬(17只中的15只)进行尸检以进行显微镜研究。在55%(6/11)的正常犬和75%(3/4)的胰腺切除犬的肝脏、肾脏、脾脏和/或胰腺中发现了大量淀粉样蛋白。淀粉样蛋白沉积物刚果红染色呈阳性,在偏振光下呈现典型的苹果绿荧光,并具有淀粉样蛋白的特征性超微结构特征。在52天内接受低至17毫克胰岛素的动物中观察到大量淀粉样蛋白沉积。在那些有肝脏淀粉样蛋白沉积的动物中,出现明显的肝肿大(即1200±250,X±标准差,而正常动物为300±25克),终末期前血清碱性磷酸酶水平明显升高(434±285,而无肝脏淀粉样蛋白沉积的动物为30±14国际单位/升)。肝脏淀粉样蛋白沉积物的量排除了它们代表胰岛素聚集体或胰岛素衍生产物本身的可能性。在胰岛素输注前获取的任何组织活检标本中均未发现淀粉样蛋白的证据。此外,鉴于犬和猪胰岛素的氨基酸序列相同,必须考虑这是否代表对注射的猪胰岛素的免疫反应。特别有趣的是,淀粉样蛋白沉积物对刚果红染色的亲和力在高锰酸钾预处理后完全消失,这表明淀粉样蛋白源自血清淀粉样蛋白A蛋白,而非免疫球蛋白轻链或胰岛素聚集体本身。该蛋白为AA型的进一步证据来自最初的生化特征分析。在6 M盐酸胍中用葡聚糖凝胶G100进行凝胶过滤,鉴定出两个分子量约为13,000和25,000道尔顿的小分子峰,两者均抑制人AA蛋白的放射免疫测定。(摘要截断于400字)
