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狒狒胎儿肺中表面活性蛋白A(SP-A)基因表达的发育及激素调控

Developmental and hormonal regulation of SP-A gene expression in baboon fetal lung.

作者信息

Seidner S R, Smith M E, Mendelson C R

机构信息

Department of Pediatrics, University of Texas Health Science Center at San Antonio 78284-7812, USA.

出版信息

Am J Physiol. 1996 Oct;271(4 Pt 1):L609-16. doi: 10.1152/ajplung.1996.271.4.L609.

Abstract

In the present study, we found that surfactant protein A (SP-A) mRNA levels, which are barely detectable in baboon fetal lung at midgestation (92 days), are increased approximately four fold between 125 and 140 days gestation, approximately 7-fold between 140 and 160 days, and approximately 1.5-fold between 160 and 174 days gestation. We also investigated the effects of dibutyryl-adenosine 3',5'-cyclic monophosphate (DB-cAMP) and dexamethasone (Dex) on SP-A gene expression in lung explants from fetal baboons at 92, 125, 140, 160, and 174 days of gestation (term = 184 days). SP-A mRNA levels, which were barely detectable in lung tissues from 92- and 125-day fetal baboons before culture, were induced after incubation for 5 days in serum-free medium and were markedly stimulated by DBcAMP. Dex caused a dose-dependent inhibition of SP-A mRNA levels and antagonized the stimulatory effect of DBcAMP. SP-A mRNA was detectable in lung tissues from 140-day fetal baboons before culture; the levels were further induced after culture and were increased greatly by DBcAMP. Again, Dex antagonized the induction of SP-A mRNA by DBcAMP. The stimulatory effects of DBcAMP and inhibitory effects of Dex on SP-A mRNA levels in lung tissues of 92- to 140-day gestational age fetal baboons were highly similar to those observed in studies using lung explants of midgestation human abortuses. By contrast, SP-A mRNA was present in relatively high levels in lung tissues of 160- and 174-day fetal baboons before culture and was relatively unaffected after incubation for 5 days in control medium. In lung explants from 160- and 174-day fetal baboons, the stimulatory effect of DBcAMP and inhibitory effect of Dex on SP-A mRNA levels were relatively modest compared with the effects of these agents on SP-A mRNA in fetal lung tissues from 92-, 125-, and 140-day gestational age fetuses. These findings suggest that, with increased lung maturation and the developmental induction of SP-A gene expression, there is a decrease in responsiveness of the fetal lung to the stimulatory effects of cAMP and inhibitory effects of glucocorticoids on SP-A gene expression.

摘要

在本研究中,我们发现表面活性蛋白A(SP-A)mRNA水平在狒狒胎儿中期妊娠(92天)的肺中几乎检测不到,在妊娠125至140天之间增加约4倍,在140至160天之间增加约7倍,在160至174天之间增加约1.5倍。我们还研究了二丁酰腺苷3',5'-环磷酸(DB-cAMP)和地塞米松(Dex)对妊娠92、125、140、160和174天(足月=184天)的狒狒胎儿肺组织外植体中SP-A基因表达的影响。在培养前,92天和125天胎儿狒狒的肺组织中几乎检测不到SP-A mRNA水平,在无血清培养基中孵育5天后被诱导,并受到DBcAMP的显著刺激。地塞米松导致SP-A mRNA水平呈剂量依赖性抑制,并拮抗DBcAMP的刺激作用。在培养前,140天胎儿狒狒的肺组织中可检测到SP-A mRNA;培养后水平进一步诱导,并因DBcAMP而大幅增加。同样,地塞米松拮抗DBcAMP对SP-A mRNA的诱导作用。DBcAMP对92至140天胎龄狒狒肺组织中SP-A mRNA水平的刺激作用和地塞米松的抑制作用与使用中期妊娠人流产肺组织外植体的研究中观察到的作用高度相似。相比之下,在培养前,160天和174天胎儿狒狒的肺组织中SP-A mRNA水平相对较高,在对照培养基中孵育5天后相对不受影响。在160天和174天胎儿狒狒的肺组织外植体中,与这些药物对92、125和140天胎龄胎儿肺组织中SP-A mRNA的影响相比,DBcAMP对SP-A mRNA水平的刺激作用和地塞米松的抑制作用相对较小。这些发现表明,随着肺成熟度增加和SP-A基因表达的发育诱导,胎儿肺对cAMP刺激作用和糖皮质激素对SP-A基因表达抑制作用的反应性降低。

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