首页> 外文期刊>Methods: A Companion to Methods in Enzymology >Differential zinc accumulation and expression of human zinc transporter 1 (hZIP1) in prostate glands.
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Differential zinc accumulation and expression of human zinc transporter 1 (hZIP1) in prostate glands.

机译:锌在前列腺中的锌积累和人类锌转运蛋白1(hZIP1)的差异表达。

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摘要

Zinc (Zn) is essential for a very large number and variety of cellular functions but is also potentially toxic. Zn homeostasis is therefore dynamically maintained by a variety of transporters and other proteins distributed in distinct cellular and subcellular compartments. Zn transport is mediated by two major protein families: the Zip family, which mediates Zn influx, and the ZnTs which are primarily linked to Zn sequestration into intracellular compartments and are, thereby, involved in lowering cytoplasmic Zn free ion concentrations. In the prostate epithelial cell, the accumulation of high cellular zinc is a specialized function that is necessary for these cells to carry out the major physiological functions of production and secretion of prostatic fluids. The loss of Zn accumulation is the most consistent and persistent characteristic of prostate malignancy. Currently, there are no direct methods to determine the relative Zn levels in various cell types of prostate gland (i.e. stroma, glandular epithelia, acini, and muscular) and no reliable ways to compare the Zn in normal versus malignant areas of the gland. Here we report a new method to show a differential Zn staining method that correlates with various stages of prostate cancer development in situ and expression of a human Zn transporter1-hZIP1 -in situ by in situ reverse transcriptase-polymerase chain reaction hybridization (ISRTPCR) that correlate with the relative Zn levels determined by the differential Zn staining method. By utilizing these methods, we show for the first time that: (1) the relative Zn levels are very low to absent in the malignant glands, (2) normal glands show high Zn levels in both glandular epithelia as well as in stromal tissues, (3) the Zn levels begin to decrease in pre-malignant glands and precedes the development of malignancy, and (4) the expression of human Zn transporter1 (hZIP1) appears to correlate with the Zn levels in the prostate glands and may be the major Zn regulator in this organ.
机译:锌(Zn)对于大量和多种细胞功能至关重要,但也可能具有毒性。因此,锌的动态平衡由分布在不同的细胞和亚细胞区室的多种转运蛋白和其他蛋白质动态维持。锌的转运由两个主要的蛋白质家族介导:介导锌流入的Zip家族和主要与Zn螯合进入细胞内区室并因此参与降低细胞质Zn游离离子浓度的ZnTs。在前列腺上皮细胞中,高细胞锌的积累是这些细胞执行生产和分泌前列腺液的主要生理功能所必需的特殊功能。锌积累的丢失是前列腺恶性肿瘤最一致和持久的特征。当前,没有直接的方法来确定前列腺的各种细胞类型(即,间质,腺上皮,腺泡和肌肉)中的相对锌水平,并且没有可靠的方法来比较正常和恶性腺区域中的锌。在这里,我们报告了一种新的方法,以显示差异锌染色方法,该方法与原位前列腺癌发展的各个阶段以及通过原位逆转录酶-聚合酶链反应杂交(ISRTPCR)原位人锌转运蛋白1-hZIP1的表达相关。与通过差异锌染色法测定的相对锌水平相关。通过使用这些方法,我们首次证明:(1)恶性腺中相对锌水平非常低,甚至不存在;(2)正常腺体在腺上皮细胞和基质组织中均显示高锌水平, (3)锌水平在恶变前腺体中开始下降并先于恶性肿瘤发展,(4)人锌转运蛋白1(hZIP1)的表达似乎与前列腺腺体中锌的水平相关,可能是主要的该器官中的锌调节剂。

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