Nitric oxide synthase isozymes antibodies.

The Histochemical Journal Pub Date : 1995-10-01
J S Pollock, U Förstermann, W R Tracey, M Nakane
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Abstract

Three isozymes of nitric oxide synthase (NOS) have been identified, cDNAs isolated and sequenced, and antibodies produced against each isozyme. Isozyme I (found primarily in central and peripheral neuronal cells), II (in cytokine-induced cells), and III (in endothelial cells) show less than 58% identity in the deduced amino acid sequences from humans. Many investigators have produced isozyme-specific antibodies and used these antibodies to locate these proteins in various cells and tissues. NOS-I is constitutively expressed, and the enzymatic activity is regulated by Ca2+ and calmodulin. The anti-NOS-I antibodies have allowed investigators to characterize non-adrenergic non-cholinergic neurons as nitrergic neurons, revealed NOS-I immunoreactivity in neurons and macula densa cells of the kidney and pancreatic islet cells, human skeletal muscle, and to demonstrate that various structures within the brain and spinal cord contain NOS-I. NOS-II is not regulated by Ca2+ and has been implicated in the pathophysiology of sepsis and autoimmune diseases. The anti-NOS-II antibodies have localized this isoform to infiltrating macrophages in pancreatic islets of diabetic rats, infiltrating macrophages and myocytes of a transplant heart model in rats, various cell types in bacterially and endotoxin-treated rats, alveolar macrophages in areas of inflammation in humans, and vascular smooth muscle cells of human atherosclerotic aneurysm. Isoform III is similar to NOS-I in that it is constitutively expressed and regulated by Ca2+ and calmodulin. Anti-NOS-III antibodies have found that this isoform is relatively specific for endothelial cells.

一氧化氮合酶同工酶抗体。
已经鉴定了一氧化氮合酶(NOS)的三种同工酶,分离了cdna并进行了测序,并产生了针对每种同工酶的抗体。同工酶I(主要存在于中枢和周围神经细胞中)、II(存在于细胞因子诱导的细胞中)和III(存在于内皮细胞中)在从人类推导的氨基酸序列中显示出不到58%的同一性。许多研究者已经制造了同工酶特异性抗体,并利用这些抗体在不同的细胞和组织中定位这些蛋白质。NOS-I是组成性表达的,酶活性受Ca2+和钙调蛋白的调控。抗NOS-I抗体使研究人员能够将非肾上腺素能、非胆碱能神经元表征为氮能神经元,揭示了NOS-I在肾脏、胰岛细胞、人类骨骼肌的神经元和黄斑致密细胞中的免疫反应性,并证明了大脑和脊髓的各种结构中含有NOS-I。NOS-II不受Ca2+的调节,并与败血症和自身免疫性疾病的病理生理有关。抗nos - ii抗体已将该亚型定位于糖尿病大鼠胰岛浸润性巨噬细胞、大鼠移植心脏模型浸润性巨噬细胞和肌细胞、细菌和内毒素处理大鼠的各种细胞类型、人类炎症区域的肺泡巨噬细胞和人类动脉粥样硬化性动脉瘤的血管平滑肌细胞。异构体III类似于NOS-I,由Ca2+和钙调蛋白组成表达和调控。抗nos - iii抗体发现这种异构体对内皮细胞具有相对特异性。
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