Institute of Human Development, Faculty of Medical and Human Sciences, University of Manchester, Manchester Academic Health Science Centre and St Mary's and Manchester Children's Hospital, Manchester, United Kingdom.
PLoS One. 2013;8(3):e57797. doi: 10.1371/journal.pone.0057797. Epub 2013 Mar 12.
Cyclic adenosine monophosphate (cAMP) drives genetic polycystic kidney disease (PKD) cystogenesis. Yet within certain PKD families, striking differences in disease severity exist between affected individuals, and genomic and/or environmental modifying factors have been evoked to explain these observations. We hypothesized that PKD cystogenesis is accentuated by an aberrant fetal milieu, specifically by glucocorticoids. The extent and nature of cystogenesis was assessed in explanted wild-type mouse embryonic metanephroi, using 8-Br-cAMP as a chemical to mimic genetic PKD and the glucocorticoid dexamethasone as the environmental modulator. Cysts and glomeruli were quantified by an observer blinded to culture conditions, and tubules were phenotyped using specific markers. Dexamethasone or 8-Br-cAMP applied on their own produced cysts predominantly arising in proximal tubules and descending limbs of loops of Henle. When applied together, however, dexamethasone over a wide concentration range synergized with 8-Br-cAMP to generate a more severe, glomerulocystic, phenotype; we note that prominent glomerular cysts have been reported in autosomal dominant PKD fetal kidneys. Our data support the idea that an adverse antenatal environment exacerbates renal cystogenesis.
环磷酸腺苷 (cAMP) 驱动遗传性多囊肾病 (PKD) 的囊泡生成。然而,在某些 PKD 家族中,受影响个体之间的疾病严重程度存在显著差异,并且已经提出了基因组和/或环境修饰因子来解释这些观察结果。我们假设 PKD 囊泡生成受到异常胎儿环境的影响,特别是糖皮质激素。通过使用 8-Br-cAMP 作为化学物质来模拟遗传 PKD 以及糖皮质激素地塞米松作为环境调节剂,评估了从野生型小鼠胚胎肾原代培养物中取出的多囊肾的扩展和性质。通过对培养条件不知情的观察者对囊泡和肾小球进行量化,并使用特定的标记物对肾小管进行表型分析。单独使用地塞米松或 8-Br-cAMP 主要在近端小管和 Henle 袢的降支中产生囊泡。然而,当一起应用时,地塞米松在广泛的浓度范围内与 8-Br-cAMP 协同作用,产生更严重的肾小球囊泡性表型;我们注意到,常染色体显性 PKD 胎儿肾脏中已经报道了明显的肾小球囊泡。我们的数据支持这样一种观点,即不利的产前环境会加剧肾脏囊泡生成。
