Cortagine: Behavioral and Autonomic Function of the Selective CRF Receptor Subtype 1 Agonist

Catherine Borna Farrokhi, Philip Tovote, Robert J. Blanchard, D. Caroline Blanchard, Yoav Litvin, Joachim Spiess
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引用次数: 26

Abstract

Corticotropin-releasing factor (CRF) is a neuropeptide and mediating component of neuroendocrine, autonomic, and behavioral processes associated with the stress response. The two receptor subtypes identified in the mammalian brain, CRF receptor subtype 1 (CRF1) and CRF2, are suggested to differentially modulate these processes. Manipulation of these receptors with selective CRF compounds and transgenic models has revealed, in most studies, a clear potentiation of the stress response through central activation of CRF1. However, pharmacological activation of CRF restricted to CRF1 has been limited by the availability of selective peptidic compounds. Recently, a highly selective CRF1 agonist, cortagine, has been developed. It was synthesized from chimeric intermediate sequences of ovine CRF, sauvagine, and human/rat CRF into a highly soluble peptide with strong affinity for CRF1 (IC50 < 5 nM) and a very low binding preference for CRF2 (IC50 > 500 nM). Affinity for the CRF binding protein (IC50 > 1,000nM) can be abolished by the addition of a glutamate residue on position 21 of the cortagine peptide sequence. Cortagine has recently been tested in a variety of preclinical models of behavior including the elevated-plus-maze (EPM), forced swim test (FST), homecage, and rat exposure test (RET). Preliminary characterization in the EPM and FST suggested that this compound elicits anxiogenic and antidepressant-like effects, respectively. Additional testing in the homecage and RET, which targets various elements of behavior, directs to a more potent anxiogenic profile of cortagine. In this review, we discuss the behavioral findings and the tests used to measure these effects. Finally, we also discuss preliminary findings of autonomic activation obtained by central injection of cortagine that support CRF1 involvement in the modulation of heart rate and heart rate variability.

Abstract Image

选择性CRF受体亚型1激动剂的行为和自主神经功能
促肾上腺皮质激素释放因子(CRF)是一种神经肽,介导与应激反应相关的神经内分泌、自主神经和行为过程。在哺乳动物大脑中发现的两种受体亚型,CRF受体亚型1 (CRF1)和CRF2,被认为对这些过程有差异调节。在大多数研究中,用选择性CRF化合物和转基因模型操纵这些受体表明,通过CRF1的中枢激活可以明显增强应激反应。然而,仅限于CRF1的CRF的药理激活受到选择性肽化合物的可用性的限制。最近,一种高选择性的CRF1激动剂cortagine被开发出来。它是由绵羊CRF、山羊CRF和人/大鼠CRF的中间序列嵌合合成的,是一种与CRF1亲和力强的高可溶性肽(IC50 <5 nM),对CRF2的结合偏好非常低(IC50 >500海里)。对CRF结合蛋白的亲和力(IC50 >1,000nM)可以通过在cortagine肽序列的第21位添加谷氨酸残基来消除。Cortagine最近在多种临床前行为模型中进行了测试,包括抬高+迷宫(EPM)、强迫游泳试验(FST)、家养和大鼠暴露试验(RET)。EPM和FST的初步表征表明,该化合物分别引起焦虑和抗抑郁样作用。在家庭和RET中进行的额外测试,针对行为的各种因素,指向了更有效的cortagine焦虑性特征。在这篇综述中,我们讨论了行为的发现和用于测量这些影响的测试。最后,我们还讨论了通过中央注射cortagine获得的自主神经激活的初步发现,这些发现支持CRF1参与心率和心率变异性的调节。
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