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头孢尼西和头孢地嗪对犬的血液学影响:人类头孢菌素血液毒性的潜在模型。

The hematologic effects of cefonicid and cefazedone in the dog: a potential model of cephalosporin hematotoxicity in man.

作者信息

Bloom J C, Lewis H B, Sellers T S, Deldar A

出版信息

Toxicol Appl Pharmacol. 1987 Aug;90(1):135-42. doi: 10.1016/0041-008x(87)90314-0.

DOI:10.1016/0041-008x(87)90314-0
PMID:3629586
Abstract

Cephalosporin antibiotics cause a variety of hematologic disturbances in man, the pathogeneses and hematopathology of which remain poorly characterized. There is a need for a well-defined animal model in which these blood dyscrasias can be studied. In four subacute toxicity studies, the intravenous administration of cefonicid or cefazedone to beagle dogs caused a dose-dependent incidence of anemia, neutropenia, and thrombocytopenia after 1-3 months of treatment. A nonregenerative anemia was the most compromising of the cytopenias and occurred in approximately 50% of dogs receiving 400-500 mg/kg cefonicid or 540-840 mg/kg cefazedone. All three cytopenias were completely reversible following cessation of treatment; the time required for recovery of the erythron (approximately 1 month) was considerably longer than that of the granulocytes and platelets (hours to a few days). Upon rechallenge with either cephalosporin, the hematologic syndrome was reproduced in most dogs tested; cefonicid (but not cefazedone)-treated dogs showed a substantially reduced induction period (15 +/- 5 days) compared to that of the first exposure to the drug (61 +/- 24 days). This observation, along with the rapid rate of decline in red cell mass parameters of affected dogs, suggests that a hemolytic component complicated the red cell production problem and that multiple toxicologic mechanisms contributed to the cytopenia. We conclude that the administration of high doses of cefonicid or cefazedone to dogs can induce hematotoxicity similar to the cephalosporin-induced blood dyscrasias described in man and thus provides a useful model for studying the mechanisms of these disorders.

摘要

头孢菌素类抗生素可在人体引起多种血液系统紊乱,但其发病机制和血液病理学特征仍不清楚。因此,需要一个明确的动物模型来研究这些血液系统异常。在四项亚急性毒性研究中,对比格犬静脉注射头孢尼西或头孢唑酮,在治疗1 - 3个月后,出现了剂量依赖性的贫血、中性粒细胞减少和血小板减少。非再生性贫血是血细胞减少症中最严重的一种,约50%接受400 - 500mg/kg头孢尼西或540 - 840mg/kg头孢唑酮治疗的犬出现该症状。停止治疗后,所有三种血细胞减少症均可完全逆转;红细胞系恢复所需时间(约1个月)比粒细胞和血小板恢复所需时间(数小时至数天)长得多。再次使用任何一种头孢菌素进行攻击,大多数受试犬都重现了血液学综合征;与首次接触药物时相比(61±24天),头孢尼西(而非头孢唑酮)治疗的犬诱导期显著缩短(15±5天)。这一观察结果,以及受影响犬红细胞质量参数的快速下降,表明溶血成分使红细胞生成问题复杂化,并且多种毒理学机制导致了血细胞减少。我们得出结论,给犬高剂量注射头孢尼西或头孢唑酮可诱导与人类中描述的头孢菌素诱导的血液系统异常相似的血液毒性,因此为研究这些疾病的机制提供了一个有用的模型。

相似文献

1
The hematologic effects of cefonicid and cefazedone in the dog: a potential model of cephalosporin hematotoxicity in man.头孢尼西和头孢地嗪对犬的血液学影响:人类头孢菌素血液毒性的潜在模型。
Toxicol Appl Pharmacol. 1987 Aug;90(1):135-42. doi: 10.1016/0041-008x(87)90314-0.
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The hematopathology of cefonicid- and cefazedone-induced blood dyscrasias in the dog.
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