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实验性镇痛剂肾病:给予连续低剂量阿司匹林和对乙酰氨基酚的Fischer 344大鼠的肾脏结构和尿液浓缩能力的变化

Experimental analgesic nephropathy: changes in renal structure and urinary concentrating ability in Fischer 344 rats given continuous low doses of aspirin and paracetamol.

作者信息

Burrell J H, Yong J L, Macdonald G J

机构信息

Department of Histology and Embryology, University of Sydney.

出版信息

Pathology. 1990 Jan;22(1):33-44. doi: 10.3109/00313029009061423.

Abstract

Long-term treatment with aspirin and paracetamol produced renal papillary necrosis in female Fischer 344 rats. Aspirin (230 mg/kg body weight/day) and paracetamol (380 mg/kg body weight/day) were dissolved in drinking water and given continuously for up to 65 weeks. Renal morphological changes were examined between 21 weeks and 65 weeks of commencement of analgesic treatment using light and electron microscopy, and were compared with age-matched controls. Structural damage initially occurred in the mid-papillary region, and specifically involved the interstitial cells and interstitial matrix. Necrosis of the epithelium of the thin limbs of the loop of Henle was present only after interstitial changes were well established. Cortical interstitial fibrosis and tubular atrophy occurred after renal papillary changes were observed. There was no evidence of significant vascular damage. Urinary concentrating ability was measured sequentially during the period of analgesic treatment. A decrease in urine concentrating ability was present when early changes to the interstitial cells and matrix were observed, and concentrating ability continued to decrease in parallel with increasing morphological damage. This study describes an animal model of analgesic-induced nephropathy, enabling early morphological changes to be studied and correlated with renal functional changes.

摘要

长期使用阿司匹林和对乙酰氨基酚对雌性Fischer 344大鼠造成了肾乳头坏死。将阿司匹林(230毫克/千克体重/天)和对乙酰氨基酚(380毫克/千克体重/天)溶解于饮用水中,连续给予长达65周。在开始镇痛治疗的21周至65周期间,使用光学显微镜和电子显微镜检查肾脏形态学变化,并与年龄匹配的对照组进行比较。结构损伤最初发生在肾乳头中部区域,特别累及间质细胞和间质基质。仅在间质变化充分确立后,才出现亨氏袢细段上皮的坏死。在观察到肾乳头变化后,出现皮质间质纤维化和肾小管萎缩。没有明显血管损伤的证据。在镇痛治疗期间依次测量尿液浓缩能力。当观察到间质细胞和基质出现早期变化时,尿液浓缩能力下降,并且随着形态学损伤的增加,浓缩能力持续下降。本研究描述了一种镇痛剂诱导的肾病动物模型,能够研究早期形态学变化并将其与肾功能变化相关联。

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