TX14(A),一种Prosaposin衍生肽,逆转链脲佐菌糖尿病大鼠的既定神经疾病,并预防半乳糖喂养大鼠的神经疾病

A. Mizisin, R. Steinhardt, J. O'Brien, N. Calcutt
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引用次数: 30

摘要

最近,一种prosaposin衍生的神经营养肽TX14(A)被证明可以预防链脲佐菌素糖尿病的大小纤维缺陷。本研究探讨了TX14(A)在链脲佐菌素糖尿病(胰岛素缺乏模型)中逆转已建立的神经传导障碍,以及在半乳糖喂养(多元醇通路通量的胰岛素充满模型)中预防神经传导障碍的功效。在注射链脲佐菌素(50 mg/kg / ip)后,一半的动物开始使用TX14(A)治疗(1 mg/kg / ip,每周3次)。8周后,一半未治疗的动物开始治疗,一半治疗的动物停止治疗,实验持续6周。TX14(A)逆转链脲唑霉素糖尿病大鼠已建立的运动和感觉神经传导缺陷,停药后3周,先前治疗的影响仍然明显。在40%半乳糖喂养开始时,给一半的对照组和一半的半乳糖喂养动物相同剂量的TX14(A),持续16周。TX14(A)在对照动物中没有效果,但它减轻了半乳糖喂养大鼠的运动和感觉神经传导缺陷,这种效果与改善坐骨神经轴突萎缩有关。这些观察结果扩展了TX14(A)的治疗效用,并强调了其在治疗糖尿病性神经病变方面的潜力。
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TX14(A), a Prosaposin‐Derived Peptide, Reverses Established Nerve Disorders in Streptozotocin‐Diabetic Rats and Prevents Them in Galactose‐Fed Rats
Recently, TX14(A), a prosaposin-derived neurotrophic peptide, was shown to prevent both large and small fiber deficits in streptozotocin diabetes. Here, the efficacy of TX14(A) in reversing established nerve conduction disorders in streptozotocin diabetes, a model of insulin deficiency, and preventing them in galactose feeding, an insulin-replete model of polyol pathway flux, was investigated. Following streptozotocin injection (50 mg/kg ip), TX14(A) treatment (1 mg/kg ip thrice weekly) was initiated in half of the animals. After 8 wk, treatment was begun in half of the untreated animals and discontinued in half of the treated animals, and the experiment continued for 6 wk. TX14(A) reversed established motor and sensory nerve conduction deficits in streptozotocin-diabetic rats and the impact of previous treatment was still evident 3 wk after withdrawal. With the onset of 40% galactose feeding, the same dose of TX14(A) was given to half of the control and half of the galactose-fed animals for 16 wk. TX14(A) was without effect in control animals but it attenuated motor and sensory nerve conduction deficits in galactose-fed rats, an effect associated with amelioration of axonal dwindling in the sciatic nerve. These observations extend the therapeutic utility of TX14(A) and highlight its potential in treating established diabetic neuropathy.
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