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黏多糖贮积症I型、VI型和VII型猫科和犬科模型中糖胺聚糖的肝脏储存情况。

Hepatic storage of glycosaminoglycans in feline and canine models of mucopolysaccharidoses I, VI, and VII.

作者信息

Haskins M E, Otis E J, Hayden J E, Jezyk P F, Stramm L

机构信息

Laboratory of Pathology, School of Veterinary Medicine, University of Pennsylvania, Philadelphia.

出版信息

Vet Pathol. 1992 Mar;29(2):112-9. doi: 10.1177/030098589202900203.

Abstract

Livers from normal cats and dogs, cats with mucopolysaccharidoses (MPS) I and VI, and dogs with MPS VII were analyzed biochemically and morphometrically to determine the lysosomal storage of glycosaminoglycans (GAG) in these animal models of human genetic disease. Analyses were performed on liver samples from seven normal cats ranging in age from 13 weeks to 15 months; six MPS I-affected cats ranging in age from 10 weeks to 26 months; four MPS VI-affected cats ranging in age from 9 months to 32 months; four normal dogs ranging in age from 1 month to 47 months; and three MPS VII-affected dogs, 5 days, 11 days, and 14 months of age. All of the animals were from the breeding colony at the University of Pennsylvania School of Veterinary Medicine and were maintained in accordance with national standards for the care and use of laboratory animals. Each GAG subclass was quantitated, and total GAG concentration was determined. Liver from cats with MPS I had the highest total GAG concentration (5.7 times that of the control), followed by liver from dogs with MPS VII (1.8 times) and cats with MPS VI (1.5 times). These data were very closely correlated (R2 = 0.982) with the results of the morphometric analyses of hepatocyte and Kupffer cell vacuolation associated with lysosomal storage and support the validity of both methods. This is particularly important for the quantification of total and individual GAG concentrations in tissue preparations. The values obtained should prove useful in future assessments of therapeutic regimes, such as enzyme replacement, bone marrow transplantation, and gene therapy, for these genetic diseases.

摘要

对正常猫和狗、患有黏多糖贮积症(MPS)I和VI的猫以及患有MPS VII的狗的肝脏进行了生化和形态计量学分析,以确定在这些人类遗传疾病动物模型中糖胺聚糖(GAG)的溶酶体储存情况。对7只年龄在13周龄至15月龄的正常猫、6只年龄在10周龄至26月龄的MPS I患病猫、4只年龄在9月龄至32月龄的MPS VI患病猫、4只年龄在1月龄至47月龄的正常狗以及3只分别为5日龄、11日龄和14月龄的MPS VII患病狗的肝脏样本进行了分析。所有动物均来自宾夕法尼亚大学兽医学院的繁殖群体,并按照国家实验室动物护理和使用标准进行饲养。对每个GAG亚类进行了定量,并测定了总GAG浓度。MPS I患病猫的肝脏总GAG浓度最高(是对照组的5.7倍),其次是MPS VII患病狗的肝脏(1.8倍)和MPS VI患病猫的肝脏(1.5倍)。这些数据与肝细胞和库普弗细胞空泡化的形态计量学分析结果密切相关(R2 = 0.982),这些空泡化与溶酶体储存有关,支持了两种方法的有效性。这对于组织制剂中总GAG和单个GAG浓度的定量尤为重要。所获得的值应证明对这些遗传疾病未来治疗方案(如酶替代、骨髓移植和基因治疗)的评估有用。

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