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新型动物源抗癌剂VRCTC-310的毒性:比格犬的急性和亚慢性研究

Toxicity of the novel animal-derived anticancer agent, VRCTC-310: acute and subchronic studies in beagle dogs.

作者信息

DeTolla L J, Stump K C, Russell R, Viskatis L J, Vidal J G, Newman R A, Etcheverry M A

机构信息

Department of Medicine (Infectious Diseases), School of Medicine, University of Maryland, Baltimore, USA.

出版信息

Toxicology. 1995 May 5;99(1-2):31-46. doi: 10.1016/0300-483x(94)02995-7.

Abstract

Acute and subchronic toxicities of VRCTC-310, a combination product of crotoxin (CT) and cardiotoxin (CD), which has shown antitumor activity in vivo, have been studied in Beagle dogs. Single i.m. doses of 0.25, 0.5 and 1.0 mg/kg resulted in dose-dependent local muscular toxicity consisting of myofiber atrophy, interstitial edema and macrophage infiltration. Also, AST, ALT and LDH levels increased on day 2, returning to normal values on days 6-8. Local lesions were absent after recovery on day 45. At 2.0 mg/kg, signs of neurotoxicity (ataxia) appeared, in addition to vomitus, salivation, hematuria and myotoxicity in tongue and diaphragm on day 8. Local lesions healed with fibrosis at the site of injection on day 45. Administration of fixed (0.025 and 0.05 mg/kg) or escalating (0.025-0.1 mg/kg) daily doses for 30 days also produced local muscular damage, which was absent at day 75. The increases in AST, ALT and LDH serum activities on days 2-4 were independent of dosing schedule and sharply decreased on day 8, despite continuation of treatment. An escalating dose schedule of 0.025-2.0 mg/kg showed local muscle damage at the site of injection on day 31, however, there were no lesions of myotoxicity in the tongue or diaphragm and no clinical signs of neurotoxicity were observed. Animals tolerated the subchronic treatment better than the acute. The resolution of serum enzymes to normal values during treatment may be attributed to a decrease of sensitivity to VRCTC-310-mediated myotoxic effects.

摘要

VRCTC - 310是一种由响尾蛇毒素(CT)和心脏毒素(CD)组成的复合产物,已在体内显示出抗肿瘤活性,本研究在比格犬中对其急性和亚慢性毒性进行了研究。单次肌肉注射剂量为0.25、0.5和1.0 mg/kg时,会产生剂量依赖性的局部肌肉毒性,表现为肌纤维萎缩、间质水肿和巨噬细胞浸润。此外,天冬氨酸转氨酶(AST)、丙氨酸转氨酶(ALT)和乳酸脱氢酶(LDH)水平在第2天升高,在第6 - 8天恢复到正常水平。在第45天恢复后局部病变消失。在2.0 mg/kg剂量时,第8天除了出现呕吐、流涎、血尿以及舌和膈肌的肌毒性外,还出现了神经毒性体征(共济失调)。在第45天,注射部位的局部病变愈合并伴有纤维化。每日给予固定剂量(0.025和0.05 mg/kg)或递增剂量(0.025 - 0.1 mg/kg)持续30天也会产生局部肌肉损伤,在第75天损伤消失。尽管继续治疗,但在第2 - 4天血清AST、ALT和LDH活性的升高与给药方案无关,并在第8天急剧下降。0.025 - 2.0 mg/kg的递增剂量方案在第31天注射部位出现局部肌肉损伤,然而,舌或膈肌未出现肌毒性病变,也未观察到神经毒性的临床体征。动物对亚慢性治疗的耐受性优于急性治疗。治疗期间血清酶恢复到正常水平可能归因于对VRCTC - 310介导的肌毒性作用的敏感性降低。

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