van Veggel K M, Huits R M H G, Donker G H, Lentjes E G W M, van Doorn J
Dept. Internal Medicine, Dr. Horacio E. Oduber Hospital, Oranjestad, Aruba; Dept. Internal Medicine, Rijnland Hospital, Leiderdorp, The Netherlands.
Dept. Internal Medicine, Dr. Horacio E. Oduber Hospital, Oranjestad, Aruba; Center for Infectious Diseases, ID4C, Military Hospital Queen Astrid, Brussels, Belgium.
Growth Horm IGF Res. 2014 Dec;24(6):233-8. doi: 10.1016/j.ghir.2014.08.002. Epub 2014 Aug 14.
Non-islet cell tumour induced hypoglycaemia (NICTH) is a paraneoplastic phenomenon that is associated with the formation of several isoforms of pro-insulin like growth factor 2 (pro-IGF-II), or so called "big" IGF-II. Disturbance of ternary complex formation by big IGF-II is assumed to be a crucial early event in the pathogenic cascade of hypoglycaemia. By size-exclusion chromatography, we investigated complex formation by adding different naturally occurring isoforms of pro-IGF-II to pooled normal adult serum. Results were compared with the analysis of the serum from a patient with NICTH.
Gel filtration experiments with the serum of a patient with NICTH demonstrated that ternary complex formation was severely compromised. The various forms of pro-IGF-II did not induce a shift of IGF-binding protein 3 (IGFBP-3) from 150kD towards smaller binary complexes in the normal adult serum, suggesting that they did not interfere with the interaction between the acid labile subunit and IGFBP-3. Instead, unglycosylated recombinant pro-IGF-II[1-104] was capable of forming a 150kD complex. In contrast, predominantly glycosylated and unglycosylated pro-IGF-II[1-87] eluted in the free unbound form. We showed that mature IGF-II and isoforms of pro-IGF-II were able to phosphorylate the IGF-I receptors of MC7 cells, albeit to a markedly lesser extent than IGF-I. When the patient's serum was tested in this system, the IGF-I receptor phosphorylation activity was considerably less than that in sera from age matched healthy individuals.
We postulate that, alongside the presence of big IGF-II in the circulation, additional steps are required to stimulate the release of IGF-II and pro-IGF-II isoforms from IGFBPs in vivo. These factors may be proteases, that are present in the local environment of the tumour and in insulin-sensitive tissues.
非胰岛细胞瘤所致低血糖症(NICTH)是一种副肿瘤现象,与胰岛素样生长因子2(pro-IGF-II)的多种异构体形成有关,即所谓的“大”IGF-II。大IGF-II干扰三元复合物形成被认为是低血糖症致病级联反应中的一个关键早期事件。通过尺寸排阻色谱法,我们将不同天然存在的pro-IGF-II异构体添加到正常成人混合血清中,研究复合物的形成情况。并将结果与一名NICTH患者的血清分析结果进行比较。
对一名NICTH患者的血清进行凝胶过滤实验表明,三元复合物的形成受到严重损害。在正常成人血清中,各种形式的pro-IGF-II并未诱导胰岛素样生长因子结合蛋白3(IGFBP-3)从150kD向较小的二元复合物转变,这表明它们并未干扰酸性不稳定亚基与IGFBP-3之间的相互作用。相反,未糖基化的重组pro-IGF-II[1-104]能够形成150kD的复合物。相比之下,主要为糖基化和未糖基化的pro-IGF-II[1-87]以游离未结合形式洗脱。我们发现,成熟IGF-II和pro-IGF-II异构体能够使MC7细胞的IGF-I受体磷酸化,尽管程度明显低于IGF-I。当在该系统中检测患者血清时,IGF-I受体磷酸化活性明显低于年龄匹配的健康个体血清中的活性。
我们推测,除了循环中存在大IGF-II外,还需要其他步骤来刺激体内IGF-II和pro-IGF-II异构体从IGFBPs中释放。这些因素可能是蛋白酶,存在于肿瘤局部环境和胰岛素敏感组织中。
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