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脑中脱氧核苷的起源:对神经发生和干细胞治疗研究的启示。

The origin of deoxynucleosides in brain: implications for the study of neurogenesis and stem cell therapy.

作者信息

Spector Reynold, Johanson Conrad E

机构信息

Robert Wood Johnson Medical School, New Brunswick, New Jersey, USA.

出版信息

Pharm Res. 2007 May;24(5):859-67. doi: 10.1007/s11095-006-9221-0. Epub 2007 Mar 20.

Abstract

Detection of DNA synthesis in brain employing ((3)H)thymidine (((3)H)dT) or bromo deoxyuridine (BrdU) is widely used as a measure of the "birth" of cells in brain development, adult neurogenesis and neuronal stem cell replacement strategies. However, recent studies have raised serious questions about whether this methodology adequately measures the "birth" of cells in brain either quantitatively or in an interpretable way in comparative studies, or in stem cell investigations. To place these questions in perspective, we review deoxynucleoside synthesis and pharmacokinetics focusing on the barriers interfacing the blood-brain (cerebral capillaries) and blood-cerebrospinal fluid (choroid plexus), and the mechanisms, molecular biology and location of the deoxynucleoside transport systems in the central nervous system. Brain interstitial fluid and CSF nucleoside homeostasis depend upon the activity of concentrative nucleoside transporters (CNT) on the 'central side' of the barrier cells and equilibrative nucleoside transporters (ENT) on their 'plasma side.' With this information about nucleoside transporters, blood/CSF concentrations and metabolic pathways, we discuss the assumptions and weaknesses of using ((3)H)dT or BrdU methodologies alone for studying DNA synthesis in brain in the context of neurogenesis and potential stem cell therapy. We conclude that the use of ((3)H)dT and/or BrdU methodologies can be useful if their limitations are recognized and they are used in conjunction with independent methods.

摘要

利用(³H)胸腺嘧啶核苷((³H)dT)或溴脱氧尿苷(BrdU)检测大脑中的DNA合成,在大脑发育、成体神经发生和神经元干细胞替代策略中作为细胞“诞生”的一种衡量方法被广泛应用。然而,最近的研究对这种方法在比较研究或干细胞研究中,是否能以一种可量化或可解释的方式充分衡量大脑中细胞的“诞生”提出了严重质疑。为了正确看待这些问题,我们回顾脱氧核苷合成和药代动力学,重点关注血脑屏障(脑毛细血管)和血脑脊液屏障(脉络丛)的界面屏障,以及中枢神经系统中脱氧核苷转运系统的机制、分子生物学和定位。脑间质液和脑脊液核苷稳态取决于屏障细胞“中枢侧”的浓缩核苷转运体(CNT)和其“血浆侧”的平衡核苷转运体(ENT)的活性。基于关于核苷转运体、血液/脑脊液浓度和代谢途径的这些信息,我们在神经发生和潜在干细胞治疗的背景下,讨论单独使用(³H)dT或BrdU方法研究大脑中DNA合成的假设和缺点。我们得出结论,如果认识到(³H)dT和/或BrdU方法的局限性,并将它们与独立方法结合使用,那么它们可能会很有用。

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