磺胺嘧啶-甲氧苄啶给药饮食对Hsd:ICR (CD1)和Tac:SW小鼠心功能、血液学和体重增加的长期影响

IF 1.1 4区农林科学 Q2 VETERINARY SCIENCES

Comparative medicine Pub Date : 2021-02-01 Epub Date: 2021-01-29 DOI:10.30802/AALAS-CM-20-000065

Nicole M Pach, Kerith R Luchins, Michael T Broman, George P Langan, Betty R Theriault

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引用次数: 0

摘要

随着心脏病和心力衰竭的惊人增加，对合适和道德的心功能障碍动物模型的需求继续增长。目前，许多心肌病动物模型需要侵入性手术或基因操作，这两种方法都需要大量的专业知识、时间和成本。我们机构的偶然发现揭示了磺胺嘧啶-甲氧苄啶(SDZ-TMP)药物饮食与IcrTac:ICR小鼠心肌病的发展之间可能存在相关性。我们假设连续饲喂SDZ-TMP给药饮食3 ~ 6个月小鼠会发生心肌细胞变性和纤维化，最终导致扩张型心肌病。共44只小鼠(22只Hsd:ICR (CD1)和22只Tac:SW)入组研究。这44只小鼠中，一半喂食标准啮齿动物饮食，另一半喂食SDZ-TMP药物饮食。基线样本，包括体重、CBCs、选择的生化参数和超声心动图，在两种饮食开始之前进行。每月获得体重，所有其他参数在研究期间至少测量一次，并在研究结束时再次测量。42周后，对小鼠实施安乐死，取心脏、肺和骨髓组织进行组织病理学检查。组织学上，对心脏的变性、纤维化、炎症和空泡化程度进行评分。数据显示，SDZ-TMP对心功能、红细胞参数、生化参数(ALT、AST、钙、镁、肌酸激酶和肌酐)、造血功能或心脏组织学评分没有显著影响。此外，随着时间的推移，喂食SDZ-TMP药物饮食的小鼠体重增加较少。总之，我们无法重现以前的发现，因此不能使用这种方法来开发一种新的心肌病模型。然而，这些结果表明，含有1365 ppm SDZ和275 ppm TMP的SDZ-TMP药物饮食似乎不会对小鼠产生长期有害影响。

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Long-Term Effects of Sulfadiazine-Trimethoprim Medicated Diet on Cardiac Function, Hematology, and Weight Gain in Hsd:ICR (CD1) and Tac:SW Mice.

With the alarming increase in heart disease and heart failure, the need for appropriate and ethical animal models of cardiac dysfunction continues to grow. Currently, many animal models of cardiomyopathy require either invasive procedures or genetic manipulation, both of which require extensive expertise, time, and cost. Serendipitous findings at our institution revealed a possible correlation between sulfadiazine-trimethoprim (SDZ-TMP) medicated diet and the development of cardiomyopathy in IcrTac:ICR mice. We hypothesized that mice fed SDZ-TMP medicated diet continuously for 3 to 6 mo would develop cardiomyocyte degeneration and fibrosis, eventually leading to dilated cardiomyopathy. A total of 44 mice (22 Hsd:ICR (CD1) and 22 Tac:SW) were enrolled in the study. Half of these 44 mice were fed standard rodent diet and the other half were fed SDZ-TMP medicated diet. Baseline samples, including weights, CBCs, select biochemistry parameters, and echocardiography were performed prior to the start of either diet. Weights were obtained monthly and all other parameters were measured at least once during the study, and again at its conclusion. After 42 wk, mice were euthanized, and heart, lung and bone marrow tissue were submitted for histopathologic evaluation. Histologically, hearts were scored for the degree of degeneration, fibrosis, inflammation, and vacuolation. The data showed that SDZ-TMP did not have a significant effect on cardiac function, RBC parameters, biochemistry parameters (ALT, AST, calcium, magnesium, creatine kinase, and creatinine), hematopoiesis, or histologic heart scores. In addition, mice fed the SDZ-TMP medicated diet gained less weight over time. In summary, we were unable to reproduce the previous findings and thus could not use this approach to develop a novel model of cardiomyopathy. However, these results indicate that SDZ-TMP medicated diet containing 1,365 ppm of SDZ and 275 ppm of TMP does not appear to have long-term detrimental effects in mice.

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来源期刊

Comparative medicine 医学-动物学

CiteScore

1.90

自引率

0.00%

发文量

审稿时长

6-12 weeks

期刊介绍： Comparative Medicine (CM), an international journal of comparative and experimental medicine, is the leading English-language publication in the field and is ranked by the Science Citation Index in the upper third of all scientific journals. The mission of CM is to disseminate high-quality, peer-reviewed information that expands biomedical knowledge and promotes human and animal health through the study of laboratory animal disease, animal models of disease, and basic biologic mechanisms related to disease in people and animals.