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The two isoforms of matrix metalloproteinase- 2 have distinct renal spatial and temporal distributions in murine models of types 1 and 2 diabetes mellitus

机译:基质金属蛋白酶2的两种同工型在1型和2型糖尿病小鼠模型中具有明显的肾脏时空分布

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We recently reported on the enhanced tubular expression of two discrete isoforms of the MMP-2 (full length and N-terminal truncated, FL-MMP-2, NTT-MMP-2) in a murine model and human diabetic kidneys. In the present study, we examined in more detail the temporal and spatial distributions of MMP-2 isoform expression in murine models of Type 1 and Type 2 diabetes mellitus. Diabetic models were streptozotocin (STZ)-induced diabetes (Type 1 diabetes mellitus) and db/db mice (Type 2 diabetes mellitus). We quantified the abundance of two isoforms of MMP-2 transcripts by qPCR. A spatial distribution of two isoforms of MMP-2 was analyzed semi-quantitatively according to time after injection of STZ and with increasing age of db/db mice. Furthermore, immunohistochemistry for nitrotyrosine was performed to examine a potential association between oxidative stress and MMP-2 isoform expression. Both isoforms of MMP-2 were upregulated in whole kidneys from STZ and db/db mice. In the case of FL-MMP-2, mRNA levels significantly increased at 12 and 24?weeks in STZ mice, while the isoform expression was significantly increased only at 16?weeks, in the db/db mice. FL-MMP-2 protein levels increased in the cortices and outer medullae of both STZ and db/db mice as a function of the duration of diabetes. For NTT-MMP-2, mRNA levels increased earlier at 4?weeks in STZ mice and at 10?weeks of age in db/db mice. The expression of NTT-MMP-2 also increased, primarily in the cortices of STZ and db/db mice, as a function of the duration of diabetes. Quantitatively, these findings were consistent with the qPCR results in the case of NTT-MMP-2, respectively (STZ 24?weeks, 3.24?±?3.70 fold; 16?weeks db/db, 4.49?±?0.55 fold). In addition, nitrotyrosine was expressed primarily in cortex as compared to medulla as a function of the duration of diabetes similar to NTT-MMP-2 expression. Two isoforms of MMP-2 are highly inducible in two diabetic murine models and become more abundant as a function of time. As the expression patterns were not the same in the two isoforms of MMP-2, it is possible that each isoform has a discrete role in the development of diabetic renal injury.
机译:我们最近报道了在鼠模型和人类糖尿病肾脏中,MMP-2的两个离散同工型(全长和N端截短,FL-MMP-2,NTT-MMP-2)的管状表达增强。在本研究中,我们更详细地检查了1型和2型糖尿病小鼠模型中MMP-2同工型表达的时空分布。糖尿病模型是链脲佐菌素(STZ)诱导的糖尿病(1型糖尿病)和db / db小鼠(2型糖尿病)。我们通过qPCR定量了MMP-2转录本的两个同工型的丰度。根据注射STZ后的时间以及随着db / db小鼠年龄的增加,半定量分析MMP-2两种同工型的空间分布。此外,进行了硝基酪氨酸的免疫组织化学检查了氧化应激和MMP-2亚型表达之间的潜在关联。在STZ和db / db小鼠的整个肾脏中,MMP-2的两种同工型均被上调。就FL-MMP-2而言,在db / db小鼠中,STZ小鼠在12和24周时mRNA水平显着升高,而同工型表达仅在16周时显着升高。 STZ和db / db小鼠的皮质和髓质中FL-MMP-2蛋白水平随糖尿病持续时间的增加而增加。对于NTT-MMP-2,STZ小鼠在4周时和db / db小鼠在10周时,mRNA的水平较早地升高。 NTT-MMP-2的表达也随糖尿病持续时间的增加而增加,主要在STZ和db / db小鼠的皮质中。从数量上看,这些发现分别与NTT-MMP-2的qPCR结果一致(STZ 24周,3.24±3.70倍; 16周db / db,4.49±0.55倍)。另外,与延髓相比,硝基酪氨酸主要在皮质中表达,这是糖尿病持续时间的函数,类似于NTT-MMP-2表达。在两个糖尿病鼠模型中,MMP-2的两个同工型是高度可诱导的,并且随着时间的推移变得更加丰富。由于在MMP-2的两个同工型中表达模式不相同,因此每种同工型在糖尿病性肾损伤的发生中可能具有离散的作用。

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