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首页> 外文期刊>Autonomic neuroscience: basic & clinical >The influences of p75 neurotrophin receptor and brain-derived neurotrophic factor in the sympathetic innervation of target tissues during murine postnatal development.
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The influences of p75 neurotrophin receptor and brain-derived neurotrophic factor in the sympathetic innervation of target tissues during murine postnatal development.

机译:p75神经营养蛋白受体和脑源性神经营养因子在鼠产后发育过程中对目标组织交感神经的影响。

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Post-ganglionic sympathetic neurons express the p75 neurotrophin receptor (p75NTR) and brain-derived neurotrophic factor (BDNF), which together have been implicated in controlling the degree of efferent innervation of peripheral organs [Kohn, J., Aloyz, R.S., Toma, J.G., Haak-Frendscho, M., Miller, F.D. 1999. Functionally Antagonistic Interactions between the TrkA and p75 Neurotrophin Receptors Regulate Sympathetic Neuron Growth and Target Innervation. J. Neurosci. 19, 5393-5408]. To examine this concept further, we developed null mutant mice lacking both p75NTR and BDNF, and assessed whether the loss of this receptor-ligand interaction negatively impacts the degree of sympathetic innervation to various target tissues. Between postnatal days 10 and 14, hearts, urinary bladders, kidneys, and submandibular salivary glands were isolated from p75(-/-)/BDNF-/-, p75-/-, BDNF-/-, and wild type siblings. Sympathetic axons were visualized using tyrosine hydroxylase (TH) immunohistochemistry, and TH protein levels were quantified by immunoblotting. Concerning the sympathetic innervation of the heart, urinary bladder and kidneys, no differences were seen in single and double null mutant mice, as compared with their wild type siblings. Sympathetic innervation of the submandibular salivary gland was, however, increased in both p75-/- and p75(-/-)/BDNF-/- mice over control mice. These results reveal that an absence of p75NTR and/or BDNF expression does not perturb the degree of sympathetic innervation of many peripheral tissues during postnatal development, and that a lack of p75NTR expression may actually enhance the density of these efferent fibers in other target tissues, such as the salivary glands.
机译:节后交感神经元表达p75神经营养蛋白受体(p75NTR)和脑源性神经营养因子(BDNF),它们共同参与控制周围器官的传出神经支配程度[Kohn,J.,Aloyz,RS,Toma, JG,Haak-Frendscho,M.,Miller,FD 1999。TrkA和p75 Neurotrophin受体之间的功能拮抗相互作用调节交感神经元的生长和目标神经。 J.神经科学。 19,5393-5408]。为了进一步检查这个概念,我们开发了同时缺乏p75NTR和BDNF的无效突变小鼠,并评估了这种受体-配体相互作用的丧失是否对各种目标组织的交感神经支配程度产生负面影响。在出生后第10至14天之间,从p75(-/-)/ BDNF-/-,p75-/-,BDNF-/-和野生型兄弟姐妹中分离出心脏,膀胱,肾脏和下颌下唾液腺。使用酪氨酸羟化酶(TH)免疫组化观察交感神经轴突,并通过免疫印迹定量TH蛋白水平。关于心脏,膀胱和肾脏的交感神经支配,与野生型同胞相比,单无效和双无效突变小鼠均未见差异。然而,与对照小鼠相比,p75-/-和p75(-/-)/ BDNF-/-小鼠中颌下唾液腺的交感神经支配都增加了。这些结果表明,缺乏p75NTR和/或BDNF表达不会干扰出生后发育过程中许多周围组织的交感神经支配程度,并且缺乏p75NTR表达实际上可能会增强其他目标组织中这些传出纤维的密度,例如唾液腺。

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