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Rat fibroblast growth factor 23 (FGF23) ELISA Kit

  • 中文名稱:
    大鼠成纖維細胞生長因子23(FGF23)酶聯免疫試劑盒
  • 貨號:
    CSB-E12170r(1)
  • 規格:
    96T/48T
  • 價格:
    ¥3600/¥2500
  • 其他:

產品詳情

  • 產品描述:
    大鼠成纖維細胞生長因子23(FGF23)酶聯免疫試劑盒(CSB-E12170r(1))為雙抗夾心法ELISA試劑盒,定量檢測血清、血漿、組織培養上清液、組織勻漿樣本中的FGF23含量。FGF23(成纖維細胞生長因子23)是一種由骨骼細胞產生的激素,通過輔因子α-Klotho與FGFR結合發揮作用,調節鈣磷代謝、維生素D代謝、PTH分泌等。研究顯示,FGF23與認知功能障礙、慢性腎病等疾病密切相關,其具體作用機制尚待進一步研究。試劑盒檢測范圍為15.6 ng/mL-1000 ng/mL,適用于體外實驗模型構建、疾病機制研究以及藥物干預效果評估等科研場景;支持科研人員高效開展內分泌代謝相關的基礎研究。本品僅用于科研,不用于臨床診斷,產品具體參數及操作步驟詳見產品說明書。
  • 別名:
    Fgf23Fibroblast growth factor 23 ELISA Kit; FGF-23 ELISA Kit
  • 縮寫:
  • Uniprot No.:
  • 種屬:
    Rattus norvegicus (Rat)
  • 樣本類型:
    serum, plasma, cell culture supernates, tissue homogenates
  • 檢測范圍:
    15.6 ng/mL-1000 ng/mL
  • 靈敏度:
    3.9 ng/mL
  • 反應時間:
    1-5h
  • 樣本體積:
    50-100ul
  • 檢測波長:
    450 nm
  • 研究領域:
    Signal Transduction
  • 測定原理:
    quantitative
  • 測定方法:
    Sandwich
  • 精密度:
    Intra-assay Precision (Precision within an assay): CV%<8%  
    Three samples of known concentration were tested twenty times on one plate to assess.
    Inter-assay Precision (Precision between assays): CV%<10%  
    Three samples of known concentration were tested in twenty assays to assess.
  • 標準曲線:

    These standard curves are provided for demonstration only. A standard curve should be generated for each set of samples assayed.

     

    ng/ml OD1 OD2 Average Corrected
    1000 2.563 2.456 2.510 2.337
    500 1.971 2.001 1.986 1.813
    250 1.243 1.289 1.266 1.093
    125 0.876 0.791 0.834 0.661
    62.5 0.486 0.472 0.479 0.306
    31.2 0.354 0.361 0.358 0.185
    15.6 0.264 0.257 0.261 0.088
    0 0.176 0.169 0.173  
  • 數據處理:
  • 貨期:
    3-5 working days

產品評價

靶點詳情

  • 最新研究進展:
    成纖維生長因子23(FGF23)是一種重要的內分泌蛋白,主要在骨骼和腎臟中合成,調節鈣磷代謝。最近的研究表明,FGF23 不僅與骨代謝異常相關,而且還與心血管、腎臟、免疫系統等多種疾病有關。例如,高水平的 FGF23 與慢性腎臟病進展、心血管疾病、骨質疏松等疾病密切相關。FGF23 的研究不斷深入,為相關疾病的治療和預防提供了新的思路。
  • 功能:
    Regulator of phosphate homeostasis. Inhibits renal tubular phosphate transport by reducing SLC34A1 levels. Regulator of vitamin-D metabolism. Negatively regulates osteoblasts differentiation and matrix mineralization. Acts directly on the parathyroid to decrease PTH secretion. Upregulates EGR1 expression in the presence of KL.
  • 基因功能參考文獻:
    1. Increases in plasma erythropoietin and erythropoietin receptor activation are mechanisms implicated in the increase of plasma FGF23 in acute kidney injury. PMID: 29395333
    2. In chronic kidney disease (CKD) rat models, FGF23 mRNA is expressed in the kidney, and the FGF23 protein is expressed at high levels in osteopontin-positive renal tubule epithelium cells likely via TGFbeta1 stimulation. FGF23 produced in the kidney might contribute to P metabolism in subjects with CKD. PMID: 29518087
    3. High FGF23 expression is associated with cardiac hypertrophy. PMID: 28339837
    4. The only direct contribution of the injured kidney to circulating FGF23 levels in uremia appears to be reduced renal extraction of bone-derived FGF23. PMID: 28341272
    5. Osteoblast Fgf23 transcription is upregulated by increase in the cytosolic Ca(2+) activity. Fgf23 transcription is decreased by Orai inhibitors and Orai1 silencing. Fgf23 transcription is lowered by NFkappaB inhibitors. PMID: 26631141
    6. EPO dependent regulation pathway of FGF23 gene expression PMID: 29073196
    7. can directly stimulate hepatic secretion of inflammatory cytokines PMID: 27457912
    8. dietary Mg deficiency causes a rapid increase in circulating levels of FGF23 and renal 24(OH)ase mRNA levels PMID: 27624533
    9. phosphate directly enhances Fgf23 transcription without affecting the stability of Fgf23 messenger RNA. PMID: 25792238
    10. Fgf23 gene transcription was abolished by the actin microfilament-disrupting agent cytochalasin B, as well as by the inhibition of actin-regulating Rac1/PAK1 signaling. PMID: 26878191
    11. Although the molecular link between the cardiac lesion and circulating Fgf23 concentrations remains to be identified, our study has uncovered a novel heart-bone-kidney axis PMID: 25858796
    12. In conclusion, PRL was responsible for the lactation-induced mucosal adaptations, which were associated with compensatory increase in FGF-23 expression probably to prevent calcium hyperabsorption. PMID: 26657069
    13. Data indicate that serum fibroblast growth factor 23 (FGF-23) levels independently correlated with bone volume parameters in rats with experimentally induced chronic kidney disease (CKD). PMID: 26186634
    14. fibroblast growth factor 23 is increased by intravenous phosphate loading in uremic rats PMID: 24625659
    15. The polycystic kidney produces FGF23 but is resistant to its action. PMID: 24402093
    16. FGF23 enhances phosphate-induced vascular calcification by promoting osteoblastic differentiation involving the ERK1/2 pathway in the absence of Klotho deficiency. PMID: 24088960
    17. Ca is not a regulator of acute changes in FGF23 secretion. PMID: 24801007
    18. data suggest that inhibition of FGFR signaling following administration of either pan-FGFR inhibitor or MEK inhibitor interferes with the FGF23 pathway, predisposing animals to hyperphosphatemia PMID: 23872713
    19. In non-iron depleted normal and uremic rats a single high dose of either of two intravenous iron preparations, iron isomaltoside 1000, and ferric carboxymaltose, had no effect on plasma levels of iFGF23 and phosphate for up to seven days. PMID: 24373521
    20. Mg deficiency increases serum FGF-23 levels. PMID: 23608165
    21. a direct and an indirect effect of parathyroid hormone on FGF23 secretion, the latter through changes in calcitriol concentrations PMID: 21525854
    22. late-onset ADHR is the product of gene-environment interactions whereby the combined presence of an Fgf23-stabilizing mutation and iron deficiency can lead to ADHR PMID: 22006328
    23. FGF23 normalizes serum phosphate and decreases 1,25-dihydroxyvitamin D levels in early-stage chronic kidney disease. PMID: 20844473
    24. Serum FGF23 increased in uremic rats treated with paricalcitol but not those treated with cinacalcet. PMID: 20200094
    25. because of a downregulation of the Klotho-FGFR1c receptor complex, an increase of circulating FGF23 does not decrease parathyroid hormone levels in established chronic kidney disease. PMID: 20016468
    26. Data indicate that cleavage at the RXXR motif abrogates FGF23 activity by removing the binding site for the binary FGFR-Klotho complex in the C-terminal region of FGF23, and by generating an endogenous inhibitor of FGF23. PMID: 19966287
    27. a feedback loop exists among serum phosphorus, 1alpha,25(OH)(2)D(3), and FGF-23, in which the novel phosphate-regulating bone-kidney axis integrated with the parathyroid hormone-vitamin D(3) axis in regulating phosphate homeostasis PMID: 15531762
    28. rat UMR-106 osteoblast-like cells were treated with 1,25(OH)(2)D(3) resulted in a dose- and time-dependent stimulation of FGF23 mRNA concentrations. PMID: 16020653
    29. Mineralized tissue cells are a principal source of Fgf23. PMID: 17350357
    30. FGF23 suppressed both parathyroid hormone (PTH) secretion and PTH gene expression PMID: 17992255
    31. These results suggest that the N- and C-terminal domains of FGF23 are responsible for association with cognate FGF receptors and Klotho, respectively, and that these interactions are indispensable for FGF23 activity. PMID: 18442315
    32. Results show that the elevated plasma FGF23 levels in uremic rats reflect the increased expression of FGF23 in bone. PMID: 19339809
    33. estrogens regulate PTH indirectly, possibly through FGF23 PMID: 19628670

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  • 亞細胞定位:
    Secreted.
  • 蛋白家族:
    Heparin-binding growth factors family
  • 組織特異性:
    Expressed in the parathyroid.
  • 數據庫鏈接:


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