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大鼠垂体前叶和中间叶中β-内啡肽相关肽的产后发育:促阿片黑素细胞皮质素加工对比发育的证据

Postnatal development of beta-endorphin-related peptides in rat anterior and intermediate pituitary lobes: evidence for contrasting development of proopiomelanocortin processing.

作者信息

Seizinger B R, Höllt V, Herz A

出版信息

Endocrinology. 1984 Jul;115(1):136-42. doi: 10.1210/endo-115-1-136.

Abstract

The concentration of immunoreactive (ir) beta-endorphin (beta-END) in the neurointermediate pituitary lobe was 15-fold higher in adult than in newborn rats; in contrast, that of ir-beta-END in the anterior lobe was twice as high in newborn as in adult animals. Ir-beta-END in the neurointermediate lobe of newborn rats consisted exclusively of beta-END-sized peptides, indicating that at birth rats are capable of processing the opioid peptide precursor proopiomelanocortin (POMC) to beta-END. Moreover, beta-END-related peptides in the neurointermediate lobe of newborn rats were found to be predominantly alpha-N-acetylated and, therefore, inactivated with respect to their opiate-like properties. Further analysis of these alpha-N-acetylated forms on high performance liquid chromatography indicated that newborn rats predominantly contained alpha-N-acetyl-(Ac-)beta-END-(1-31), whereas the major forms in adult rats were Ac-beta-END-(1-27) and -(1-26). Thus, the C-terminal processing of Ac-beta-END-(1-31) to -(1-27) and -(1-26) may not yet be fully active at birth, in contrast to the processing of POMC to beta-END. In the anterior lobe of newborn rats, however, the ratio of beta-lipotropin/beta-END resembled that of adults, and more than 80% of beta-END-sized ir-material was found to consist of nonacetylated (and therefore opiate-active) beta-END-(1-31), as in adults, suggesting that the enzymatic system responsible for processing of POMC to beta-lipotropin and beta-END is already mature at birth. The high concentrations of beta-END in the anterior lobe of newborn rats suggest a possible role of this opioid peptide in perinatal development and/or parturition.

摘要

成年大鼠神经垂体中叶中免疫反应性(ir)β-内啡肽(β-END)的浓度比新生大鼠高15倍;相反,前叶中ir-β-END的浓度在新生动物中是成年动物的两倍。新生大鼠神经垂体中叶中的ir-β-END仅由β-END大小的肽组成,这表明出生时大鼠能够将阿片肽前体阿黑皮素原(POMC)加工成β-END。此外,发现新生大鼠神经垂体中叶中与β-END相关的肽主要是α-N-乙酰化的,因此就其类阿片特性而言是无活性的。在高效液相色谱上对这些α-N-乙酰化形式的进一步分析表明,新生大鼠主要含有α-N-乙酰基-(Ac-)β-END-(1-31),而成年大鼠中的主要形式是Ac-β-END-(1-27)和-(1-26)。因此,与POMC加工成β-END不同,Ac-β-END-(1-31)的C末端加工成-(1-27)和-(1-26)在出生时可能尚未完全活跃。然而,在新生大鼠的前叶中,β-促脂素/β-END的比例与成年大鼠相似,并且发现超过80%的β-END大小的ir物质由非乙酰化(因此具有阿片活性)的β-END-(1-31)组成,与成年大鼠一样,这表明负责将POMC加工成β-促脂素和β-END的酶系统在出生时已经成熟。新生大鼠前叶中β-END的高浓度表明这种阿片肽在围产期发育和/或分娩中可能发挥作用。

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