In adult kidney donors a range of responses to loss of a kidney have been observed ranging from maintenance of renal function and blood pressure,[5, 6] to low incidence of renal failure[61] and moderate elevations in blood pressure,[62] to overt hypertension, proteinuria and reduced GFR.[8, 43, 63] In a meta-analysis of normotensive adult kidney donors, Boudville et al. reported a 5 mmHg Sotrastaurin greater increase
in arterial pressure over 5–10 years post donation in donors compared with age-matched individuals with intact kidneys.[9] Although this may seem a negligible increase in blood pressure, it should be noted that with every 2 mmHg decrease in arterial pressure, the risks of advanced cardiovascular diseases are significantly reduced.[64] Moreover, stratification by race/ethnicity has revealed a greater risk for hypertension and chronic kidney disease in kidney donors of African American origin compared with Caucasian Americans[65] and also compared with the population of non-donor African Americans.[66] Another important factor that may determine the differences in response to loss of renal mass is the
initial nephron number. In humans, there is a 10-fold range in normal nephron number.[1] Therefore, it is plausible that donors who develop renal and cardiovascular dysfunction may have started out at the lower end of the nephron number spectrum compared with those who GSK2118436 cope well with loss of a kidney. In children who are born with only one kidney, glomerular hyperfiltration is evident as GFR in the first two decades of life increases to levels similar to that of children born with two kidneys.[67] Although renal function is restored in the early stages of life, a decline in GFR and renal functional reserve have been observed after the second decade of life in children with a solitary functioning kidney.[58, 68, 69] However, this decline in renal function is not always associated with hypertension or renal disease. In some studies long-term follow-up of patients has revealed a reduction in GFR, and the presence
of albuminuria and hypertension, in children with Niclosamide a solitary kidney.[7, 70, 71] Approximately 30% of these children develop end-stage renal disease early in adulthood,[7, 67] some as early as 18 years of age.[72]Conversely, stable renal function with no excess incidence of hypertension and proteinuria has also been observed.[73, 74] Furthermore, the degree of renal hypertrophy may serve as a prognostic marker for elevation in blood pressure, since in children with a solitary kidney, the percentage increase in length of the kidney correlates well with the percentage increase in blood pressure.[71] It also appears that in some instances, secondary factors may be necessary to unmask the negative effects of a nephron deficit.