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异丙肾上腺素刺激大鼠垂体神经中间叶体外释放β-内啡肽及相关肽:某些分子形式的β-内啡肽优先释放的证据。

Isoproterenol-stimulated release of beta-endorphin and related peptides from the rat pituitary neurointermediate lobe in vitro: evidence for preferential release of certain molecular forms of beta-endorphin.

作者信息

Sweep C G, Boersma C J, Wiegant V M

机构信息

Rudolf Magnus Institute, Department of Pharmacology, Medical Faculty, University of Utrecht, The Netherlands.

出版信息

Neuropeptides. 1990 Oct;17(2):63-73. doi: 10.1016/0143-4179(90)90051-y.

Abstract

The intermediate lobe of the pituitary gland synthesizes the multifactorial precursor molecule pro-opiomelanocortin (POMC), from which, through a process of post-translational enzymatic processing, beta-endorphin-(1-31) (beta E) and a variety of N alpha-acetylated and C-terminally shortened forms of this peptide are generated. Using an in vitro superfusion system, the release of these endorphins from intact rat neurointermediate lobes (NILs) was investigated under basal and isoproterenol (ISO) stimulated conditions. Superfusion of NILs with the beta-adrenergic agonist ISO (30 min pulse) resulted in a rapid, sustained and concentration-dependent stimulation of the release of beta E-like immunoreactivity (beta E-IR) over basal as determined with an antiserum directed against the C-terminus of the beta E- (1-31) sequence (10(-6) M: + 145%; 10(-7) M: + 73%; 10(-8) m: + 41%). The release of N(alpha)-acetylated-endorphin-like immunoreactivity (AcE-IR) was stimulated to a similar extent. These effects of ISO were antagonized by the competitive alpha-adrenoceptor antagonist propranolol in a concentration-dependent manner, indicating the involvement of alpha-adrenoceptors. The beta-related peptides released from the NILs under basal and ISO-stimulated conditions were further characterized, based on their retention times in a reversed-phase HPLC system and their reactivity with specific antisera recognizing respectively the midportion of beta E, the N-terminus of acetylated endorphins, the C-terminus of tau-endorphin (beta E-(1-17); tau E), or the C-terminus of alpha-endorphin (beta E-(1-16); alpha E). In HPLC fractionated superfusates 10 peaks were resolved that reacted with the midportion beta E antiserum. In superfusates collected under basal conditions, three major peaks possessed chromatographical and immunological characteristics of Ac beta E-(1-26), Ac beta E- (1-27) Ac beta E-(1-31). In addition, a prominent peak was found eluting around the retention time of beta E-(1-31), that contained both acetylated and non-acetylated material. Six smaller peaks were observed, with the characteristics of beta E-(1-26) and beta E-(1-27) (these peptides were not resolved with the HPLC system used), Ac tau E, tau E, Aa alpha E, and des-tyrosine-alpha E (DT alpha E), respectively. In superfusates collected during superfusion of NILs with ISO (10(-6) M) all peaks were increased. However, those eluting as beta E-(1-31), beta E-(1-26)/beta E-(1-27), Ac beta E-(1-26) and Ac tau E appeared to be preferentially stimulated.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

垂体中间叶合成多因子前体分子阿片促黑激素皮质素原(POMC),通过翻译后酶促加工过程,可产生β-内啡肽-(1-31)(βE)以及该肽的多种Nα-乙酰化和C末端缩短形式。利用体外灌注系统,研究了在基础条件和异丙肾上腺素(ISO)刺激条件下,这些内啡肽从完整大鼠神经中间叶(NILs)的释放情况。用β-肾上腺素能激动剂ISO(30分钟脉冲)灌注NILs,导致βE样免疫反应性(βE-IR)的释放迅速、持续且呈浓度依赖性地高于基础水平,这是用针对βE-(1-31)序列C末端的抗血清测定的(10⁻⁶ M:+ 145%;10⁻⁷ M:+ 73%;10⁻⁸ M:+ 41%)。Nα-乙酰化内啡肽样免疫反应性(AcE-IR)的释放也受到类似程度的刺激。ISO的这些作用被竞争性α-肾上腺素能拮抗剂普萘洛尔以浓度依赖性方式拮抗,表明α-肾上腺素能受体参与其中。基于它们在反相高效液相色谱系统中的保留时间以及与分别识别βE中部、乙酰化内啡肽N末端、τ-内啡肽(βE-(1-17);τE)C末端或α-内啡肽(βE-(1-16);αE)C末端的特异性抗血清的反应性,对基础条件和ISO刺激条件下从NILs释放的β相关肽进行了进一步表征。在高效液相色谱分离的灌注液中,分辨出10个与βE中部抗血清反应的峰。在基础条件下收集的灌注液中,三个主要峰具有AcβE-(1-26)、AcβE-(1-27)、AcβE-(1-31)的色谱和免疫特征。此外,在βE-(1-31)的保留时间附近发现一个突出峰,其中包含乙酰化和非乙酰化物质。观察到六个较小的峰,分别具有βE-(1-26)和βE-(1-27)(这些肽在用的高效液相色谱系统中未分离)、AcτE、τE、AaαE和去酪氨酸-αE(DTαE)的特征。在用ISO(10⁻⁶ M)灌注NILs期间收集的灌注液中,所有峰均增加。然而,以βE-(1-31)、βE-(1-26)/βE-(1-27)、AcβE-(1-26)和AcτE形式洗脱的峰似乎受到优先刺激。(摘要截断于400字)

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