Anti-LPIN3 OTI1C8;Mouse mAb

Anti-LPIN3 OTI1C8;Mouse mAb

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  • 询价
  • DIMA
  • DME908112
  • 2025年07月15日
  • Mouse
  • Human
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    • 详细信息
    • 技术资料
    • 亚型

      IgG1

    • 形态

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    • 保存条件

      Store at -20°C

    • 标记物

      Unconjugated

    • 适应物种

      Human

    • 保质期

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    • 级别

      仅用于科研

    • 库存

      1 week

    • 宿主

      Mouse

    • 浓度

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    • 靶点

      LPIN3

    • 规格

      100ul

    背景 Humans lipodystrophy is characterized by loss of body fat, fatty liver, hypertriglyceridemia, and insulin resistance. Mice carrying mutations in the fatty liver dystrophy (fld) gene have similar phenotypes. Through positional cloning, the mouse gene responsible for fatty liver dystrophy was isolated and designated Lpin1. The nuclear protein encoded by Lpin1 was named lipin. Lpin1 mRNA was expressed at high levels in adipose tissue and was induced during differentiation of preadipocytes. These results indicated that lipin is required for normal adipose tissue development and provided a candidate gene for human lipodystrophy. Through database searches, mouse and human EST and genomic sequences with similarities to Lpin1 were identified. These included two related mouse genes (Lpin2 and Lpin3) and three human homologs (LPIN1, LPIN2, and LPIN3). Human LPIN1 gene has been mapped to 2p25.; linkages of fat mass and serum leptin levels to this same region have been noted. Human LPIN2 and LPIN3 mapped to chromosomes 18p11 and 20q11-q12, respectively. The mouse genes encoding Lpin1, Lpin2, and Lpin3 mapped to chromosome 12, 17, and 2, respectively. [provided by RefSeq, Jul 2008]
    别名 LIPN3L; SMP2
    推荐稀释比 WB 1:2000
    组分&重悬 PBS (pH 7.3) containing 1% BSA, 50% glycerol and 0.02% sodium azide.
    纯化 Purified from mouse ascites fluids or tissue culture supernatant by affinity chromatography (protein A/G)
    Uniprot ID Q9BQK8

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