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SDS
犬腎損傷分子1(Kim1)酶聯(lián)免疫吸附試劑盒
Catalog #: E08K0025
Sample Type: Biological samples

 

Other Names

Canine Kidney Injury Molecule 1 ELISA kit

HAVCR1; TIM1; TIMD1; HAVCR; Hepatitis A Virus Cellular Receptor 1; T Cell Immunoglobulin And Mucin Domain-Containing Protein 1; T-cell immunoglobulin mucin receptor 1

Research Area

Immunology, Microbiology

Background

The kidney injury molecule-1 (designated as Kim-1 in rodents, KIM-1 in humans) mRNA was identified using techniques of representational difference analysis, a PCR-based technique, which we carried out to find genes whose expression was markedly upregulated 24–48 h after ischaemia in the rat. Kim-1 was the gene found to be most highly upregulated in this screen. A large pharmaceutical company consortium, using an unbiased genomic approach to evaluate genes upregulated with the nephrotoxin cisplatin, determined that Kim-1 was upregulated more than any other of the 30 000 genes tested. There are a large number of studies in animals showing robust Kim-1 protein production in the affected segments of the proximal tubule whenever a toxin or pathophysiological state results in dedifferentiation of the epithelium. Dedifferentiation is a very early manifestation of the epithelial cell response to injury. KIM-1 is also expressed, at much lower levels, in lymphocytes and has also been referred to as T-cell immunoglobulin mucin (TIM)-1 and HAVCR-1, hepatitis A virus cellular receptor-1. The protein has also been reported to be expressed in the cochlea in response to cisplatin-induced injury . The KIM/TIM family consists of eight members in mice, six in rats and three in humans.