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间歇性与连续性给予神经生长因子对大鼠基底前脑内侧隔胆碱能神经元损伤的影响

Intermittent vs Continuous Administration of Nerve Growth Factor to Injured Medial Septal Cholinergic Neurons in Rat Basal Forebrain.

作者信息

Miller Kenneth E, Frierdich Gregory E, Dillard Robert H, Soriano Robert H, Roufa Dikla G

机构信息

Department of Anatomy and Cell Biology, Oklahoma State University Center for Health Sciences, Tulsa, USA.

出版信息

Neurosci Med. 2014 May;5(2):109-118. doi: 10.4236/nm.2014.52014. Epub 2014 Apr 30.

Abstract

Many medial septal neurons of the basal forebrain are dependent on nerve growth factor (NGF) from the hippocampus for survival and maintenance of a cholinergic phenotype. When deprived of their source of NGF by axotomy, medial septal neuronal cell bodies atrophy and lose their cholinergic markers. This is similar to what is observed in the basal forebrain during Alzheimer's disease (AD). In the present study, medial septal neurons were axotomized in female rats by way of a fimbria/fornix lesion. For fourteen days following axotomy, varying NGF doses (1 - 250 μg/ml) were administered to the lateral cerebral ventricle with either mini-osmotic infusion or daily injection. The responsiveness of medial septal neurons was evaluated with choline acetyltransferase immunohistochemistry. Within the mini-osmotic pumps, NGF activity diminished greatly during the first five days of implantation, but increased dramatically in the CSF after five days of infusion. The responsiveness of medial septal neurons to NGF was dose dependent and the ED for NGF injection was determined to be 14.08 μg/ml compared to 27.60 μg/ml for NGF infusion. Intermittent injections at varying intervals were evaluated with 30 μg/ml NGF over a fourteen-day time period (2, 3, 6, or 12 injections). No differences occurred in the number of choline acetyltransferase neurons from rats that received weekly injections to those that received daily injections of NGF. NGF administration has been suggested as a therapy for AD. The results of these studies continue to highlight the need for NGF stability within the delivery system and AD patient CSF, the choice of delivery system, frequency of administration, and the NGF dose for maintaining basal forebrain cholinergic neurons during AD.

摘要

基底前脑的许多内侧隔区神经元依赖海马体分泌的神经生长因子(NGF)来维持生存及胆碱能表型。通过切断轴突剥夺其NGF来源后,内侧隔区神经元细胞体会萎缩并失去胆碱能标记物。这与阿尔茨海默病(AD)患者基底前脑的情况相似。在本研究中,通过切断穹窿/穹窿海马纤维对雌性大鼠的内侧隔区神经元进行轴突切断。轴突切断后的14天内,通过微量渗透泵输注或每日注射,向侧脑室给予不同剂量(1 - 250μg/ml)的NGF。用胆碱乙酰转移酶免疫组织化学法评估内侧隔区神经元的反应性。在微量渗透泵内,植入后的前5天NGF活性大幅下降,但输注5天后脑脊液中的NGF活性显著增加。内侧隔区神经元对NGF的反应呈剂量依赖性,NGF注射的半数有效剂量为14.08μg/ml,而NGF输注的半数有效剂量为27.60μg/ml。在14天的时间内(2、3、6或12次注射),用30μg/ml的NGF评估不同间隔的间歇性注射。接受每周注射NGF的大鼠与接受每日注射NGF的大鼠相比,胆碱乙酰转移酶神经元数量没有差异。有人提出将NGF给药作为AD的一种治疗方法。这些研究结果继续凸显了在给药系统和AD患者脑脊液中保持NGF稳定性、给药系统的选择、给药频率以及在AD期间维持基底前脑胆碱能神经元所需的NGF剂量的必要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/09ba/6247915/a761c6361d8b/nihms-994959-f0001.jpg

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