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Remote Communication through Solute Carriers and ATP Binding Cassette Drug Transporter Pathways: An Update on the Remote Sensing and Signaling Hypothesis

机译:通过溶质载体和ATP结合盒式药物转运蛋白途径的远程通讯:遥感和信号假说的更新。

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摘要

Recent data from knockouts, human disease, and transport studies suggest that solute carrier (SLC) and ATP binding cassette (ABC) multispecific “drug” transporters maintain effective organ and body fluid concentrations of key nutrients, signaling molecules, and antioxidants. These processes involve transcellular movement of solutes across epithelial barriers and fluid compartments (e.g., blood, cerebrospinal fluid, urine, bile) via “matching” or homologous sets of SLC (e.g., SLC21, SLC22, SLC47) and ABC transporters. As described in the “Remote Sensing and Signaling Hypothesis” (Biochem Biophys Res Commun >323:429–436, 2004; Biochem Biophys Res Commun >351:872–876, 2006; J Biol Chem >282:23841–23853, 2007; Nat Clin Pract Nephrol >3:443–448, 2007; Mol Pharmacol >76:481–490, 2009), highly regulated transporter networks with overlapping substrate preferences are involved in sensing and signaling to maintain homeostasis in response to environmental changes (e.g., substrate imbalance and injury). They function in parallel with (and interact with) the endocrine and autonomic systems. Uric acid (urate), carnitine, prostaglandins, conjugated sex steroids, cGMP, odorants, and enterobiome metabolites are discussed here as examples. Xenobiotics hitchhike on endogenous carrier systems, sometimes leading to toxicity and side effects. By regulation of the expression and/or function of various remote organ multispecific transporters after injury, the overall transport capacity of the remote organ to handle endogenous toxins, metabolites, and signaling molecules may change, aiding in recovery. Moreover, these transporters may play a role in communication between organisms. The specific cellular components involved in sensing and altering transporter abundance or functionality depend upon the metabolite in question and probably involve different types of sensors as well as epigenetic regulation.
机译:基因敲除,人类疾病和运输研究的最新数据表明,溶质载体(SLC)和ATP结合盒(ABC)多特异性“药物”转运蛋白可维持重要营养素,信号分子和抗氧化剂的有效器官和体液浓度。这些过程涉及溶质通过“匹配”或同源的SLC组(例如SLC21,SLC22,SLC47)和ABC转运蛋白跨上皮屏障和液室(例如血液,脑脊髓液,尿液,胆汁)的跨细胞运动。如“遥感和信号假说”中所述(Biochem Biophys Res Commun > 323: 429-436,2004; Biochem Biophys Res Commun > 351: 872-876,2006; J Biol Chem > 282:,2007年; Nat Clin Pract Nephrol > 3: 443-448,2007年; Mol Pharmacol > 76: 481– (第490页,2009年),具有重叠的底物偏好的高度监管的运输网络参与传感和信号传递,以维持对环境变化(例如,底物失衡和伤害)的动态平衡。它们与内分泌和自主系统平行(并相互作用)。此处以尿酸(尿酸盐),肉碱,前列腺素,共轭性类固醇,cGMP,增味剂和肠生物体代谢产物为例进行讨论。异种生物在内源性载体系统上搭便车,有时会导致毒性和副作用。通过调节损伤后各种远端器官多特异性转运蛋白的表达和/或功能,远端器官处理内源性毒素,代谢产物和信号分子的总转运能力可以改变,有助于恢复。此外,这些转运蛋白可能在生物之间的交流中发挥作用。涉及传感和改变转运蛋白丰度或功能的特定细胞成分取决于所讨论的代谢物,可能涉及不同类型的传感器以及表观遗传调控。

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