首页> 外文期刊>American Journal of Physiology >Peripherally administered desacetyl alpha-MSH and alpha-MSH both influence postnatal rat growth and associated rat hypothalamic protein expression.
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Peripherally administered desacetyl alpha-MSH and alpha-MSH both influence postnatal rat growth and associated rat hypothalamic protein expression.

机译:外周给予的脱乙酰基α-MSH和α-MSH均会影响出生后大鼠的生长以及相关的大鼠下丘脑蛋白表达。

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摘要

Desacetyl alpha-MSH predominates over alpha-MSH during development, but whether it is biologically active and has a physiological role is unclear. We compared the effects of 0.3 microg.g(-1).day(-1) desacetyl alpha-MSH with that of 0.3 microg.g(-1).day(-1) alpha-MSH on postnatal body growth by administering the peptides subcutaneously daily for postnatal days 0-14 and also used a two-dimensional gel electrophoresis gel-based proteomic approach to analyze protein changes in hypothalami, the relay center for body weight and growth regulation, after 14 days of treatment. We found that the growth rate between days 1 and 10 was significantly decreased by desacetyl alpha-MSH but not by alpha-MSH, but by day 14, a time reported for development of a mature pattern of hypothalamic innervation, both peptides had significantly increased neonatal growth compared with PBS-treated control rats. Desacetyl alpha-MSH significantly increased spleen weight, but alpha-MSH had no effect. alpha-MSH significantly decreased kidney weight, but desacetyl alpha-MSH had no effect. Both desacetyl alpha-MSH and alpha-MSH significantly decreased brain weight. By 14 days, both peptides significantly changed expression of a number of hypothalamic proteins, specifically metabolic enzymes, cytoskeleton, signaling, and stress response proteins. We show that peripherally administered desacetyl alpha-MSH is biologically active and induces responses that can differ from those for alpha-MSH. In conclusion, desacetyl alpha-MSH appears to be an important regulator of neonatal rat growth.
机译:在发育过程中,脱乙酰基α-MSH比α-MSH占优势,但是尚不清楚它是否具有生物活性并具有生理作用。我们比较了0.3 microg.g(-1).day(-1)脱乙酰基α-MSH和0.3 microg.g(-1).day(-1)alpha-MSH对出生后身体生长的影响在产后0到14天每天皮下注射肽,并在治疗14天后使用基于二维凝胶电泳凝胶的蛋白质组学方法分析下丘脑中的蛋白质变化,下丘脑是体重和生长调节的中继中心。我们发现,去乙酰α-MSH可显着降低第1天至第10天之间的生长速率,但α-MSH并不会显着降低生长速率,但到第14天(据报道发育成熟的下丘脑神经支配方式的时间),两种肽均显着增加了新生儿与PBS处理的对照大鼠相比,其生长快。脱乙酰基α-MSH明显增加了脾脏重量,但是α-MSH没有作用。 α-MSH显着降低了肾脏重量,但是去乙酰基α-MSH没有作用。脱乙酰基α-MSH和α-MSH均可显着降低大脑重量。到14天时,这两种肽都显着改变了许多下丘脑蛋白的表达,特别是代谢酶,细胞骨架,信号传导和应激反应蛋白。我们表明,外围给予的去乙酰α-MSH具有生物活性,并诱导可能不同于α-MSH的反应。总之,脱乙酰基α-MSH似乎是新生大鼠生长的重要调节剂。

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