Cell and Transport Physiology Antidiuretic Effect of Hydrochlorothiazide in Lithium-Induced Nephrogenic Diabetes Insipidus is Associated With Upregulation of Aquaporin-2, Na-Cl Cotransporter and Epithelial Sodium Channel Regulating H2O Transport: Effects of Thiazide Diuretics.
Clinical conditions (lithium, hypercalcemia,etc.) with impaired water reabsorption in nephrogenic diabetesinsipidus (NDI) and decreased Aquaporin-2 abundance. Thiazidediuretics blunt the polyuria in NDI, an effect attributed tovolume contraction, reduced glomerular filtration and enhancedproximal reabsorption. The studies by Kim et al. in this issue,provide a better understanding of the effects of thiazide diureticsin lithium-induced NDI, which include a well-coordinated increasein the sodium transport capacity (NaCl cotransporters and epithelialsodium channels), as well as Aquaporin-2 in the aldosterone-responsivedistal nephron. Enhance water reabsorption via Aquaporin-2 requiresan increase in medullary tonicity, yet NaCl cotransporter expressionis usually ascribed to the cortical diluting segments. The responseto hydrochlorothiazide is concentration of the urine and reducedurine volume, implying that increased salt transport in theconcentrating segments (thick ascending limb), perhaps mediatedby vasopressin, also plays an important role in this responseto thiazide diuretics. Page 2836
Genetics and Development WT1 Activates a Glomerular-Specific Enhancer Identified from the Human Nephrin Gene Toward a Better Podocyte. Using the Nephrin Promoter to Overexpress Proteins in a Podocyte Specific Fashion.
Quests to better understand theglomerular barrier to protein filtration have taken on manyforms over the past several decades from the purely structuralusing transmission electron microscopy, to the functional withemphasis on size and charge-selective properties of the filterto now molecular with the recognition that a mutation in theslit diaphragm protein nephrin underlies congenital nephroticsyndrome. The nephrin story has sparked an avalanche of researchto identify, establish function for and eventually to manipulatesuch missing or abnormal proteins that underlie what are nowtermed "podocytopathies". Quaggin et al. colleagues lead usfurther toward that goal by identifying a 183 base pair segmentthat is homologous between the human and mouse nephrin promotersand showing that it can be utilized to express a test proteinin a podocyte specific distribution in transgenic mice, andthat the tumor suppressor gene WT1 enhances that expression.The paper is an important technical advance, and the intensityof the podocyte protein expression achieved is nicely illustratedin this month’s cover photo. Page 2851
Basic Mineral Metabolism Human Vascular Smooth Muscle Cells Undergo Vesicle-Mediated Calcification in Response to Changes in Extracellular Calcium and Phosphate Concentrations Higher Extracellular Calcium Concentrations Induce Calcification in Vascular Smooth Muscle Cells. Or Does Calcium Induce Vascular Calcification.
Cardiovascular disease is the leadingcause of death among hemodialysis patients and disorders ofmineral metabolism have been linked to vascular calcificationin epidemiological studies. Vascular calcification has beenascribed to supersaturation of calcium and phosphorus and subsequentprecipitation. More recently, investigators have demonstratedcalcification to be an active process, potentially exacerbatedor inhibited by serum factors. Reynolds et al. demonstrate thatmodest elevations in extracellular calcium and phosphorus concentrationsindependently and synergistically induce human vascular smoothmuscle cell calcification by release of membrane-bound matrixvesicles in viable cells and apoptotic bodies in dying cells.Exposure to serum diminish, and pre-treatment of vascular smoothmuscle cells with warfarin enhance, vesicle calcification. Thesedata bring us several steps closer to understanding the processof vascular calcification, and toward understand the mechanism(s)by which chronic kidney disease contributes to the process.Page 2857
Pathophysiology of Renal Disease and Progression Hepatocyte Growth Factor Ameliorates Renal Interstitial Inflammation in Rat Remnant Kidney by Modulating Tubular Expression of MCP-1 and RANTES Attacking Renal Inflammation in CKD.
Hepatocyte growth factor (HGF) isemerging as an impressive anti-fibrotic agent based on reportsthat it attenuates chronic renal injury in several experimentalmodels. How does it work? The initial studies demonstrated HGFeffects on the production of pro-fibrotic growth factors suchas TGF-(. However, more recent studies have identified directeffects of HGF that might prevent chronic kidney damage suchas enhanced degradation of extracellular matrix and blockadeof tubular epithelial-to-mesenchymal transition to interstitialmyofibroblasts. The study by Gong et al. in this issue of JASN,uncovers a new aspect of HGF biology that is highly relevantto progressive kidney disease. Using a rat remnant kidney model,administration of exogenous HGF significantly reduced tubularchemokine production (MCP-1 and RANTES) and the number of interstitialmacrophages and was associated with reduced kidney fibrosis,proteinuria and serum creatinine levels. Neutralization of endogenouslyproduced HGF had the reverse outcome. In vitro studies confirmedthat HGF inhibited MCP-1 and RANTES production by cultured tubularcells. There is a significant body of literature supportinga direct relationship between activated interstitial macrophagesand progressive kidney disease. HGF therapy can be added tothe growing list of therapeutic strategies that might preventCKD by suppressing that interstitial inflammatory response tochronic injury. Page 2868
Basic Transplantation Selectin Inhibitor Bimosiamose Prolongs Survival of Kidney Allografts by Reduction in Intragraft Production of Cytokines and Chemokines Inhibiting Selectins in Experimental Renal Transplantation.
In this manuscript, Langer et al.studied the effects of selectin ligand inhibition on kidneyallograft survival in an experimental model of renal transplantationin rats. They show that administration of the selectin inhibitorBimosiamose prevents acute rejection and increases allograftsurvival in this model. Importantly, the agent was also synergisticwith existing immunosuppressive agents in promoting graft survival.The effect was associated with decreased expression of chemokinesand cytokines in the graft. Although the exact mechanism ofaction of this novel agent is not defined this is a potentiallyclinically relevant manuscript. Future work should focus ondefining exact mechanism of action, studying its effect on chronicrejection and translating its effect to a large animal modeland ultimately humans. Page 2893
CLINICAL SCIENCE
Epidemiology and Outcomes Association of Chronic Kidney Disease and Anemia with Physical Capacity: The Heart and Soul Study It’s Not Just Anemia that Makes CKD Patients Tired.
Both severe anemia and advancedchronic kidney disease (CKD) have been associated with decreasedexercise capacity. In this issue, Odden et al. have addressedthese associations in patients with coronary artery diseasefrom the Heart and Soul Study. Among 954 eligible patients,24% had a creatinine clearance <60 ml/min and 9% had Hb <12g/L. Compared to patients with higher values, patients witheither anemia or CKD had lower self-reported physical functionand lower objective exercise capacity. Subjects with both anemiaand CKD had lower physical function and exercise capacity thanpatients with either condition alone. Among patients with coronaryartery disease, moderately severe CKD and anemia appear to beindependently associated with decreased physical capacity. Page2908
Effect of an Increase in CRP Level During a Hemodialysis Session on Mortality Can Measuring CRP Predict Death in Dialysis Patients?
Inflammation, estimated by serumC-reactive protein (CRP), is associated with worse clinicaloutcomes in patients treated with dialysis. In this issue, Korevaaret al. report that, among hemodialysis patients with an elevatedserum CRP concentration, an increase in serum CRP (>0.5mg/L)during a single hemodialysis treatment was associated with anincreased risk of death. For each 1 mg/L CRP increase, therewas a 9% increased mortality risk. The independent patient relatedvariables associated with an increase in serum CRP were increasedage and low serum cholesterol while the dialysis related variableswere higher dialysate flow rate and use of two dialysis needles.The 2 yr survival rate was 66% for the group without an increasein CRP compared to 44% for those with an increase (P = 0.09).These data should stimulate a search for dialysis related variables,which might be causally associated and amenable to change. Page2916
Clinical Dialysis Racial and Center Differences in Hemodialysis Adequacy in Children Treated at Pediatric Centers: A NAPRTCS Report Is There Racial Bias in Dialysis Delivery to Kids?
The North American Pediatric RenalTransplant Cooperative Study (NAPRTCS) group has made a majorcontribution to understanding the prevalence of adequacy ofhemodialysis in children treated with hemodialysis in NorthAmerica. Adequate dialysis, defined as >75% of calculatedKt/V values greater >1.2, was achieved in 70% of the patientsevaluated. The statistically significant predictors of inadequatedialysis dose were male gender, black race, larger body surfacearea and absence of Kt/V reporting at a center. The study limitationsincluded participation of 50% of eligible centers, the potentialfor selection bias and a relatively small final sample size.Nevertheless, this study identified inadequate dialysis in about30% of these patients and demonstrated gender and racial disparitiesin achieving target Kt/V values. Page 2923
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