Receptor mediated endocytosis of hemoglobin-haptoglobin, galactosylated serum albumin and polymeric IgA by the liver.

Acta biologica et medica Germanica Pub Date : 1982-01-01
J N Limet, J Quintart, C Otte-Slachmuylder, Y J Schneider
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Abstract

Labelled hemoglobin-haptoglobin (ham-hap), galactosylated serum albumin (gal-SA) and polymeric immunoglobulin A (p IgA) were injected intravenously to rats or mice. The labels disappeared from the plasma with a half-time of about 5 min and were almost entirely found associated with the liver where degradation products progressively appear. The uptake of hem-hap and gal-SA are partially saturable as a function of the plasmatic concentration and the uptake of gal-SA can be completely inhibited by the simultaneous injection of asialofetuin. About 45 min after injection to rats, labelled material appears in the bile in amounts corresponding to 3.9% of the injected dose (hem-hap), 2.8% (gal-SA) and 60.1% (p IgA). The molecular weight of the labelled material transferred into the bile has been characterized: it consists almost entirely of intact IgA and for about 60% of intact hem-hap and gal-SA. Cell fractionation experiments indicate that 4 min after injection, the label is associated with components which equilibrate around a density of 1.13 g/cm3 and which dissociate from marker enzymes of Golgi complex, plasma membrane and lysosomes. Longer times after injection (from 20 min for hem-hap and gal-SA to 1 h for p IgA) labelled material appears, within lysosomes. To explain all these data, we suggest that after binding to plasma membrane receptors, the ligands are rapidly interiorized into pinocytic vesicles which fuse with lysosomes. Most of the hem-hap and gal-SA molecules but only part of p IgA would be released and subsequently digested; these vesicles would dissociate from lysosomes and fuse with the biliary membrane where the molecules still bound to the membrane of the vesicles would be detached and excreted into the bile.

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受体介导的肝内吞血红蛋白-接触珠蛋白、半乳糖化血清白蛋白和聚合IgA。
大鼠或小鼠静脉注射标记血红蛋白-接触珠蛋白(ham-hap)、半乳糖化血清白蛋白(gal-SA)和聚合免疫球蛋白A (p IgA)。这些标签在大约5分钟的半衰期从血浆中消失,并且几乎完全与肝脏相关,在肝脏中降解产物逐渐出现。作为血浆浓度的函数,hema -hap和gal-SA的摄取是部分饱和的,同时注射asialofetuin可以完全抑制gal-SA的摄取。大鼠注射后约45分钟,胆汁中出现标记物质,其数量分别为注射剂量的3.9% (hem-hap)、2.8% (gal-SA)和60.1% (p - IgA)。转移到胆汁中的标记物质的分子量已被表征:它几乎完全由完整的IgA和大约60%完整的hemp -hap和gal-SA组成。细胞分离实验表明,注射后4分钟,该标记与密度在1.13 g/cm3左右平衡的组分相关,这些组分与高尔基复合体、质膜和溶酶体的标记酶解离。注射后较长时间(hemp -hap和gal-SA为20分钟,p - IgA为1小时)溶酶体内出现标记物质。为了解释所有这些数据,我们认为在与质膜受体结合后,配体迅速内化成与溶酶体融合的胞质囊泡。大部分的hemhap和gal-SA分子会被释放并随后被消化,但只有一部分的p - IgA分子会被消化;这些囊泡将与溶酶体分离并与胆道膜融合,在胆道膜上仍然结合的分子将被分离并排泄到胆汁中。
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