延长早产儿和低出生体重婴儿肾发生的治疗概念必须与肾发生区的结构-功能特性相对应。

IF 2.4 Q1 PEDIATRICS
Will W Minuth
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引用次数: 3

摘要

许多研究都涉及哺乳动物肾脏的标本和肾单位的初级发育。然而,只有很少的信息是关于肾脏发育的最后步骤,导致出生时肾源区形态原活性下调和器官被膜外排列的干细胞龛的损失。令人惊讶的是,这些发育过程中的自然变化与早产儿和低出生体重婴儿的肾脏发生的过程相似。尽管这些婴儿出生时肾源区基本完整,生态位活跃,但他们中的很大一部分患有肾生成障碍,导致少肾病、非典型肾小球的形成和实质不成熟。本研究指出,目前尚未确定的肾源区noxae阻碍了实质发育的初级步骤。在这种情况下,一个可能的治疗目标是通过药物延长肾脏形成。然而,实际数据提供的信息表明,由于肾源区出乎意料的复杂显微解剖,药物的给药是有问题的,到目前为止,还没有考虑到细胞外基质的纹理和间充质细胞突起与上皮干细胞之间通过隧道纳米管的特殊接触。因此,形态因子信号的干扰是否会改变细胞外基质的合成、细胞间接触的干扰或间质液的改变是否会损害肾形成活性,仍有待研究。由于大多数尚未解决的问题,寻找符合条件的延长肾脏发生的药物及其可靠的给药是未来的一个特殊挑战。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Concepts for a therapeutic prolongation of nephrogenesis in preterm and low-birth-weight babies must correspond to structural-functional properties in the nephrogenic zone.

Concepts for a therapeutic prolongation of nephrogenesis in preterm and low-birth-weight babies must correspond to structural-functional properties in the nephrogenic zone.

Concepts for a therapeutic prolongation of nephrogenesis in preterm and low-birth-weight babies must correspond to structural-functional properties in the nephrogenic zone.

Concepts for a therapeutic prolongation of nephrogenesis in preterm and low-birth-weight babies must correspond to structural-functional properties in the nephrogenic zone.

Numerous investigations are dealing with anlage of the mammalian kidney and primary development of nephrons. However, only few information is available about the last steps in kidney development leading at birth to a downregulation of morphogen activity in the nephrogenic zone and to a loss of stem cell niches aligned beyond the organ capsule. Surprisingly, these natural changes in the developmental program display similarities to processes occurring in the kidneys of preterm and low-birth-weight babies. Although those babies are born at a time with a principally intact nephrogenic zone and active niches, a high proportion of them suffers on impairment of nephrogenesis resulting in oligonephropathy, formation of atypical glomeruli, and immaturity of parenchyma. The setting points out that up to date not identified noxae in the nephrogenic zone hamper primary steps of parenchyma development. In this situation, a possible therapeutic aim is to prolong nephrogenesis by medications. However, actual data provide information that administration of drugs is problematic due to an unexpectedly complex microanatomy of the nephrogenic zone, in niches so far not considered textured extracellular matrix and peculiar contacts between mesenchymal cell projections and epithelial stem cells via tunneling nanotubes. Thus, it remains to be figured out whether disturbance of morphogen signaling altered synthesis of extracellular matrix, disturbed cell-to-cell contacts, or modified interstitial fluid impair nephrogenic activity. Due to most unanswered questions, search for eligible drugs prolonging nephrogenesis and their reliable administration is a special challenge for the future.

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