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小鼠体内甲醛加合物的放射自显影成像:对糖尿病血管损伤的潜在意义

Autoradiographic imaging of formaldehyde adducts in mice: possible relevance for vascular damage in diabetes.

作者信息

Grönvall J L, Garpenstrand H, Oreland L, Ekblom J

机构信息

Department of Neuroscience (Pharmacology), Uppsala University, Biomedical Center, Sweden.

出版信息

Life Sci. 1998;63(9):759-68. doi: 10.1016/s0024-3205(98)00331-2.

Abstract

The activity of semicarbazide-sensitive amine oxidase (SSAO) has been reported to be elevated in blood from diabetic patients. It has been suggested that the enzyme is involved in the development of complications such as retinopathies, nephropathies and neuropathies, which are associated with advanced diabetes, possibly by the formation of toxic metabolites. Under the influence of SSAO, methylamine is deaminated to formaldehyde which is known to react with various macromolecules. It has therefore been proposed that specific inhibition of SSAO could be of therapeutic value for treatment of diabetic patients. The present results provide evidence that treatment with an SSAO inhibitor potently reduces the levels of irreversible adducts. In this study, 14C-methylamine was given intraperitoneally to NMRI mice, and the tissue distribution of irreversibly bound methylamine metabolites was estimated by an autoradiographic method. Such radioactive residues occurred in high concentrations in the intestinal wall, brown adipose tissue, spleen and bone marrow. By inhibiting SSAO irreversibly with hydralazine before giving 14C-methylamine to the mice, it was possible to determine the resynthesis rate of SSAO in different tissues. A complete recovery of SSAO activity was seen in the intestinal wall after 6 days, whereas only about 60% was recovered in adipose tissue after 14 days. This suggests that factors controlling the synthesis of SSAO differ in these tissues, or that these tissues express different forms of enzymes.

摘要

据报道,糖尿病患者血液中氨基脲敏感胺氧化酶(SSAO)的活性升高。有人认为,该酶可能通过形成有毒代谢产物参与了与晚期糖尿病相关的并发症,如视网膜病变、肾病和神经病变的发生发展。在SSAO的作用下,甲胺脱氨生成甲醛,已知甲醛会与各种大分子发生反应。因此,有人提出特异性抑制SSAO可能对糖尿病患者的治疗具有治疗价值。目前的结果提供了证据,表明用SSAO抑制剂治疗可有效降低不可逆加合物的水平。在本研究中,将14C-甲胺腹腔注射给NMRI小鼠,并通过放射自显影法估计不可逆结合的甲胺代谢产物的组织分布。这种放射性残留物在肠壁、棕色脂肪组织、脾脏和骨髓中高浓度出现。在给小鼠注射14C-甲胺之前,用肼不可逆地抑制SSAO,可以确定不同组织中SSAO的再合成速率。6天后肠壁中SSAO活性完全恢复,而14天后脂肪组织中仅恢复约60%。这表明控制SSAO合成的因素在这些组织中不同,或者这些组织表达不同形式的酶。

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