A Primer on Congenital Anomalies of the Kidneys and Urinary Tracts (CAKUT)

Murugapoopathy, Vasikar; Gupta, Indra R.

doi:10.2215/cjn.12581019

Cited by 129 publications

(117 citation statements)

References 61 publications

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“…In addition to reduced nephron, impaired nephrogenesis can cause a wide spectrum of defects in the kidney and urinary tract, namely congenital anomalies of the kidney and urinary tract (CAKUT) [ 35 ]. Unlike adults, CAKUT is one of the major causes of CKD in children [ 36 ].…”

Section: Developmental Origins Of Cvd and Kidney Disease: Human Evidencementioning

confidence: 99%

Preventive Aspects of Early Resveratrol Supplementation in Cardiovascular and Kidney Disease of Developmental Origins

Hsu

Hou

Tain

2021

IJMS

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The increase in the incidence of cardiovascular diseases (CVDs) and kidney disease has stimulated research for strategies that could prevent, rather than just treat, both interconnected disorders. Resveratrol, a polyphenolic compound with pleiotropic biofunctions, has shown health benefits. Emerging epidemiological data supports that early life environmental insults are regarded as increased risks of developing CVDs and kidney disease in adulthood. Conversely, both disorders could be reversed or postponed by shifting interventions from adulthood to earlier stage by so-called reprogramming. The purpose of this review is first to highlight current epidemiological studies linking cardiovascular and renal programming to resulting CVD and kidney disease of developmental origins. This will be followed by a summary of how resveratrol could exert a positive influence on CVDs and kidney disease. This review also presents an overview of the evidence documenting resveratrol as a reprogramming agent to protect against CVD and kidney disease of developmental origins from animal studies and to outline the advances in understanding the underlying molecular mechanisms. Overall, this review reveals the need for future research to further clarify the reprogramming effects of resveratrol before clinical translation.

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Section: Developmental Origins Of Cvd and Kidney Disease: Human Evidencementioning

confidence: 99%

Preventive Aspects of Early Resveratrol Supplementation in Cardiovascular and Kidney Disease of Developmental Origins

Hsu

Hou

Tain

2021

IJMS

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“…The major developmental events include UB formation, UB branching morphogenesis, formation of bladder and kidney, kidney tubule branching, and nephrogenesis [ 49 ]. Impaired branching morphogenesis and nephrogenesis can cause low nephron endowment and a spectrum of defects in the kidney and urinary tract, namely congenital anomalies of the kidney and urinary tract (CAKUT) [ 50 ]. The developing kidneys are vulnerable to environmental risk factors that impair development throughout gestation: a malformed kidney is a severe defect happening during early pregnancy, whereas defects that occur later are generally less severe [ 50 ].…”

Section: Developmental Origins Of Kidney Diseasementioning

confidence: 99%

Developmental Origins of Kidney Disease: Why Oxidative Stress Matters?

Hsu

Tain

2020

Antioxidants

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The “developmental origins of health and disease” theory indicates that many adult-onset diseases can originate in the earliest stages of life. The developing kidney has emerged as being particularly vulnerable to adverse in utero conditions leading to morphological and functional changes, namely renal programming. Emerging evidence indicates oxidative stress, an imbalance between reactive oxygen/nitrogen species (ROS/RNS) and antioxidant systems, plays a pathogenetic role in the developmental programming of kidney disease. Conversely, perinatal use of antioxidants has been implemented to reverse programming processes and prevent adult-onset diseases. We have termed this reprogramming. The focus of this review is twofold: (1) To summarize the current knowledge on oxidative stress implicated in renal programming and kidney disease of developmental origins; and (2) to provide an overview of reprogramming effects of perinatal antioxidant therapy on renal programming and how this may prevent adult-onset kidney disease. Although early-life oxidative stress is implicated in mediating renal programming and adverse offspring renal outcomes, and animal models provide promising results to allow perinatal antioxidants applied as potential reprogramming interventions, it is still awaiting clinical translation. This presents exciting new challenges and areas for future research.

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“…The corollary to this strategy is a prediction that unless severe, most subjects with low nephron number will not develop ESRD until after peak reproductive years, when selection pressure is low. 109 Consistent with this prediction, a Norwegian study of over 2 million subjects revealed that low birth weight, IUGR, and preterm birth represent cumulative risk factors for development of ESRD that is delayed until later adulthood. 110 The aging kidney.…”

Section: Metabolic Control Of Nephron Numbermentioning

confidence: 84%

“…108 Congenital anomalies of the kidneys and urinary tracts can result from genomic, epigenomic, or environmental stressors in any combination, and the more severe the nephron deficit, the sooner the onset of CKD and the more rapid its progression. 109 Human life history strategy favors allocation of energy to the developing brain through physiologic adaptation by the fetal cerebral circulation, 53 and by metabolic regulation of organ development by nuclear and mitochondrial gene transcription regulated epigenetically (Fig. 4).…”

Section: Metabolic Control Of Nephron Numbermentioning

confidence: 99%

Bioenergetic Evolution Explains Prevalence of Low Nephron Number at Birth: Risk Factor for CKD

Chevalier

2020

Kidney360

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There is greater than tenfold variation in nephron number of the human kidney at birth. Although low nephron number is a recognized risk factor for CKD, its determinants are poorly understood. Evolutionary medicine represents a new discipline that seeks evolutionary explanations for disease, broadening perspectives on research and public health initiatives. Evolution of the kidney, an organ rich in mitochondria, has been driven by natural selection for reproductive fitness constrained by energy availability. Over the past 2 million years, rapid growth of an energy-demanding brain in Homo sapiens enabled hominid adaptation to environmental extremes through selection for mutations in mitochondrial and nuclear DNA epigenetically regulated by allocation of energy to developing organs. Maternal undernutrition or hypoxia results in intrauterine growth restriction or preterm birth, resulting in low birth weight and low nephron number. Regulated through placental transfer, environmental oxygen and nutrients signal nephron progenitor cells to reprogram metabolism from glycolysis to oxidative phosphorylation. These processes are modulated by counterbalancing anabolic and catabolic metabolic pathways that evolved from prokaryote homologs and by hypoxia-driven and autophagy pathways that evolved in eukaryotes. Regulation of nephron differentiation by histone modifications and DNA methyltransferases provide epigenetic control of nephron number in response to energy available to the fetus. Developmental plasticity of nephrogenesis represents an evolved life history strategy that prioritizes energy to early brain growth with adequate kidney function through reproductive years, the trade-off being increasing prevalence of CKD delayed until later adulthood. The research implications of this evolutionary analysis are to identify regulatory pathways of energy allocation directing nephrogenesis while accounting for the different life history strategies of animal models such as the mouse. The clinical implications are to optimize nutrition and minimize hypoxic/toxic stressors in childbearing women and children in early postnatal development.

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A Primer on Congenital Anomalies of the Kidneys and Urinary Tracts (CAKUT)

Cited by 129 publications

References 61 publications

Preventive Aspects of Early Resveratrol Supplementation in Cardiovascular and Kidney Disease of Developmental Origins

Preventive Aspects of Early Resveratrol Supplementation in Cardiovascular and Kidney Disease of Developmental Origins

Developmental Origins of Kidney Disease: Why Oxidative Stress Matters?

Bioenergetic Evolution Explains Prevalence of Low Nephron Number at Birth: Risk Factor for CKD

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