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Ki-67和BrdU作为成体神经发生增殖标志物的效用。

The utility of Ki-67 and BrdU as proliferative markers of adult neurogenesis.

作者信息

Kee N, Sivalingam S, Boonstra R, Wojtowicz J M

机构信息

Department of Physiology, Medical Sciences Building, University of Toronto, Ont., Canada M5S 1A8.

出版信息

J Neurosci Methods. 2002 Mar 30;115(1):97-105. doi: 10.1016/s0165-0270(02)00007-9.

Abstract

Adult animals continue to produce new neurons in the dentate gyrus of hippocampus. Until now, the principal method of studying neurogenesis has been to inject either tritiated thymidine or 5'-Bromo-2-deoxyuridine (BrdU) intraperitoneally followed by autoradiographic or immunohistochemical detection methods respectively. However, such exogenous markers may produce toxic effects. Our objective was to determine whether Ki-67, a nuclear protein expressed in all phases of the cell cycle except the resting phase, can be used as an alternative, endogenous marker. Using immunohistochemistry, we examined Ki-67 and BrdU expression pattern in rats. Ki-67 was expressed within the proliferative zone of the dentate gyrus and its expression pattern mimicked that of BrdU when examined soon after exogenous BrdU administration. Quantitative comparison of BrdU and Ki-67-positive cells showed 50% higher numbers of the latter when examined 24 h after the BrdU injection. This was expected, since BrdU can be incorporated into DNA only during the S-phase of the mitotic process, whereas Ki-67 is expressed for its whole duration. Experimental increases (by ischemia) or reductions (by radiation) in the number of mitotic cells produced parallel changes in BrdU and Ki-67 signals. Thus, Ki-67 is an effective mitotic marker and has most of the benefits of BrdU and none of the costs. This study provides evidence for Ki-67 to be used as a marker of proliferation in the initial phase of adult neurogenesis.

摘要

成年动物的海马齿状回会持续产生新的神经元。到目前为止,研究神经发生的主要方法是分别腹腔注射氚标记胸腺嘧啶核苷或5'-溴-2'-脱氧尿苷(BrdU),随后分别采用放射自显影或免疫组织化学检测方法。然而,这类外源性标记物可能会产生毒性作用。我们的目的是确定Ki-67(一种在细胞周期除静止期外的所有阶段均有表达的核蛋白)是否可作为一种替代性的内源性标记物。我们采用免疫组织化学方法检测了大鼠体内Ki-67和BrdU的表达模式。Ki-67在齿状回的增殖区内表达,在外源性给予BrdU后不久进行检测时,其表达模式与BrdU相似。对BrdU和Ki-67阳性细胞进行定量比较发现,在注射BrdU后24小时检测时,后者的数量比前者高50%。这是意料之中的,因为BrdU仅在有丝分裂过程的S期才能掺入DNA,而Ki-67在整个细胞周期均有表达。有丝分裂细胞数量的实验性增加(通过缺血)或减少(通过辐射)会使BrdU和Ki-67信号产生平行变化。因此,Ki-67是一种有效的有丝分裂标记物,具有BrdU的大部分优点且无其缺点。本研究为Ki-67可作为成年神经发生初始阶段增殖的标记物提供了证据。

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