Cell and Transport Physiology Investigations of Pharmacologic Properties of the Renal CLC-K1 Chloride Channel Co-expressed with Barttin by the Use of 2-(p-Chlorophenoxy)Propionic Acid Derivatives and Other Structurally Unrelated Chloride Channel Blockers Are New Diuretics on the Horizon?
Diuretics are important in the multidrug approach needed toreach blood pressure targets in patients with chronic kidneydisease. Loop agents and thiazides interact with apical membraneNa+ transporters. New approaches can be focused on the mechanismsby which NaCl is transported across the basolateral membrane.Chloride channels (CLC-K1 and CKC-K2) have gained prominencein this regard, underscored by genetic defects that can affectthese channels (Bartter syndrome and perhaps some cases of Gitelmansyndrome). Liantonio et al. describe the interactions amongCLC-K1, its accessory beta subunit (barttin), and chlorophenoxy-propionicacid derivatives. Structure-activity relations are explored,and it is noted that this class of agents is effective fromthe basolateral (blood) side of the cells. The potency of thecurrent generation of agents is not yet adequate to considertheir clinical utility, but this approach may be worthwhilein developing new therapeutic agents with diuretic potential.Page13
Cell Biology Angiotensin II Type 1-Receptor Mediated Changes in Heparan Sulfate Proteoglycans in Human SV40 Transformed Podocytes The Effect of ACE Inhibition on Proteinuria May Not Be Entirely Hemodynamic.
Although the role of AngII in regulating post-glomerular resistanceand intraglomerular pressure is well known, there has been anexpanding literature on AngII effects that are independent ofhemodynamics and that may contribute to renal disease. Theseinclude induction of interstitial disease and fibrosis, effectson TGF-, and several others. In this article, Brinkkoeter etal. examine AngII effects on podocyte production of negativelycharged heparan sulfate proteoglycans (HSPG), molecules thatconstitute a major portion of the negative charge barrier toprotein filtration. They find a marked decrease in both celland matrix HSPG associated with AngII expression. These changescould explain the loss of the charge barrier in proteinuricdiseases like diabetic nephropathy, and they also contributeto the reduction of proteinuria seen with AngII inhibitors,which could presumably restore the charge barrier as well asreduce intraglomerular pressure.Page 33
Hemodynamics and Vascular Regulation Oxidant Stress Leads to Impaired Regulation of Renal Cortical Oxygen Consumption by Nitric Oxide in the Aging Kidney Oxidant Stress and Aging - YES or NO?
This study examines regulation of renal oxygen consumption inthe aging rat kidney. Specifically, this study shows decreasedability of the aged rat to regulate oxygen consumption via NOproduction. The finding is reversed by the super oxide dismutasemimetic tempol and the NAD(P)H oxidase inhibitor Apocynin, indirectlysuggesting that super oxide production from NAD(P)H oxidasewas the reason for decreased NO bioavailability. While thisreport provides evidence in support of the first of two possibilities,it remains unresolved from this and other reports of decreasedrenal NO in aging animals whether it is indeed increased oxidativestress that quenches NO or decreased NO production that is mostresponsible for the exaggeration of the harmful effects of oxidativestress that cause renal injury in aging. Definition of the relativeimportance of these two pathophysiologic scenarios continuesto be a challenge for future studies.Page 52
Immunology and Pathology Podocytes Populate Cellular Crescents in a Murine Model of Inflammatory Glomerulonephritis Are Podocytes Previously Unrecognized Contributors to Glomerular Crescent Formation?
Crescents represent the clinician’s nightmare: the signof severe capillary wall injury and usually a rapid and oftenirreversible loss of renal function. Previously regarded asreflecting only a proliferation of parietal epithelial cellslining Bowman’s capsule, we now recognize that crescentsmark disruption not only in glomerular basement membrane butalso in Bowman’s capsule and have a multicellular compositionthat includes monocytes and fibroblasts derived from the interstitiumand parietal epithelial cells. Further insight into the compositionof crescents is provided by this study, which uses podocyte-specificmarkers and transgenic mice to establish that up to 25% of cellspopulating glomerular crescents in the mouse are actually derivedfrom podocytes, although they lack podocyte-specific markers.However, mice are not humans, and the remarkable podocyte proliferationthat occurs in nephritic mouse glomeruli after deposition ofthis antibody is unique, raising the question of whether thesestructures are truly crescents in the traditional sense. Morework will be required to show that a similar process occursin human disease.Page 61
Pathophysiology of Renal Disease and Progression Prevention of Acute Ischemic Renal Failure by Targeted Delivery of Growth Factors to the Proximal Tubule in Transgenic Mice: The Efficacy of Parathyroid Hormone-Related Protein and Hepatocyte Growth Factor Why Do Diabetic Glomeruli Have So Much Extracellular Matrix?
One of the principal pathologic features of diabetic nephropathyis the excess of extracellular matrix in the form of both expandedmesangial matrix and thickening of glomerular basement membrane(GBM). While considerable attention has been given to the roleof mesangial cells in diabetic nephropathy, the GBM thickeningis presumably a consequence of podocyte dysfunction, a considerablyless-studied area. Adler et al. from Harbor-UCLA provide convincingdata from both cell-culture and whole-animal studies to showthat exposure to high glucose stimulates the 12-lipoxygenasepathway in podocytes, which signals the p38-Map kinase pathwayto activate synthesis of the -5 chain of type IV collagen. Thefact that changes similar to those observed in cell culturewere also documented in the intact diabetic animal providesstrong evidence that the in vitro observations are relevantto what occurs in vivo. While the complex processes that regulatematrix synthesis and degradation in the GBM are certainly morecomplicated than this, the study does provide novel informationon the role of glucose in the pathogenesis of diabetic nephropathy.The next step will be to see if this process can be amelioratedwith 12-lipoxygenase inhibitors such as nonsteroidal antiinflammatoryagents.Page 112
Basic Dialysis Glycosaminoglycans Enhance the Trifluoroethanol-Induced Extension of 2-Microglobulin-Related Amyloid Fibrils at a Neutral pH From 2 Microglobulin to Amyloid - A Role for GAGs?
It is now well known that 2-microglobulins can form amyloidand that this has been an important source of morbidity complicatingdialysis therapy. This study uses a reagent, trifluoroethanol,that induces the extension of 2-microglobulin-related amyloidfibrils under experimental conditions. Despite not normallybeing found in the body, the effect of trifluoroethanol in thisexperimental setting demonstrates the possibility that potentiallyother more biologically relevant agents may denature specificproteins enough to permit amyloid fibril formation at physiologicpH. The fact that glycosaminoglycans accelerate this processis of interest, implying that cell surface heparan sulfate proteoglycanscould contribute to the process of 2-microglobulin amyloid formation.Page126
CLINICAL SCIENCE
Clinical Nephrology Timing of Complications in Percutaneous Renal Biopsy What Is the Optimal Time to Observe Patients for Complications after Renal Biopsy?
For all of us who do percutaneous renal biopsies on native kidneys,as well as for those who refer such patients to radiologists,the issue of how long a patient must be observed after biopsyto ensure that complications have not occurred is an importantone. Clinical lore suggests that 8 to 12 h is reasonable, whichused to result in overnight stays in the hospital. However,emphasis on cost control has reduced that period to a few hoursin most centers. This article from a busy and experienced groupat Rush-Presbyterian-St. Luke’s Hospital in Chicago providesdata on complication rates in 750 patients biopsied with modernreal-time ultrasound technology and spring-loaded needles. Itdocuments a higher complication rate in patients with renalinsufficiency and provides good data to justify an observationperiod of up to 24 h after biopsy.Page 142
Effects of Early and Late Intervention with Epoetin on Left Ventricular Mass among Patients with Chronic Kidney Disease (Stage 3 or 4): Results of a Randomized Clinical Trial EPO-Does It Also Improve the Heart?
A report by Roger et al. in this issue of JASN describes a carefullydesigned and conducted clinical trial that examined the effectof anemia correction on the development and progression of leftventricular hypertrophy (LVH) among patients with moderate tosevere chronic kidney disease (CKD). The result of the trialwas unexpected, and no differences were noted in left ventricularmass index (LVMi) or progression of LVH between the erythropoietin-treatedand comparison groups. The authors note that the expected separationin hemoglobin levels was not achieved during the study, withmean hemoglobin of 122 ± 7 g/L in the intervention groupand 110 ± 10 g/L in the control group. Further, few patientsin the intervention (50%) or the comparison (19%) arms actuallyachieved the planned hemoglobin levels. Among those subjectswho did achieve protocol targets, changes in LVMi were consistentwith previous studies. Overall, the 2-yr LVMi increase in thetreated subjects was 44% less than that observed in the controlsubjects, 2.5 ± 20 g/m2versus 4.5 ± 20 g/m2 (difference,2.0 g/m2; 95% CI, -8.4 to 4.0; P = 0.44). On the basis of theseobservations, the authors estimate that a study would need atotal of 1571 patients to demonstrate a significant differencebetween groups achieving this degree of separation in hemoglobinlevels. Clearly, this small multicenter study illustrates theneed for larger trials of the anemia/LVH hypothesis and raisesimportant issues about the design of future interventions. Untilevidence from more and larger studies is available, the roleof anemia correction in the management of cardiovascular diseaserisk in the pre-ESRD phase of CKD will remain uncertain.Page148
Dialysis Factors that Affect Postdialysis Rebound in Serum Urea Concentration, Including the Rate of Dialysis: Results from the HEMO Study What Are the Determinats of How Much Rebound in BUN Occurs after Dialysis?
Daugirdas et al. present a detailed analysis of the variablesthat affect the postdialysis rebound in serum urea concentration.The equilibrated Kt/V has been estimated as a linear functionof single pool Kt/V and the rate of dialysis (K/V). Data from1331 HEMO study subjects identified greater urea rebound inAfrican-American patients, male patients, those without congestiveheart failure, those with greater age, those with higher ultrafiltrationrate, and those with low predialysis or intradialysis systolicblood pressure. Optimum values for the slope term (B) were determinedfor arteriovenous access and for venous catheters at two samplingtimes: immediate and 20 s after dialysis. The authors suggestthat variability associated with other factors is consistentwith a regional blood flow model of urea kinetics.Page 194
Transplantation Proteomic-Based Detection of Urine Proteins Associated with Acute Renal Allograft Rejection A Dipstick Test for Acute Rejection? The Promise of Proteomics—Almost!
The quest for development of biological markers of renal allograftdysfunction and novel non-invasive diagnostic tools for renalallograft rejection led Schaub et al. to perform an interestingstudy exploring protein clusters by mass spectrometry of urinesamples. The results identified a unique cluster in the majorityof rejecting recipients but not in normals or other groups whoare either stable or have dysfunction due to ischemia or glomerulopathy.This is a cross-sectional study, and the data require prospectivevalidation to define predictive value and utility in surveillanceand interventions. More importantly, the data will stimulatefurther research aimed at identifying the proteins and leadingto development of novel therapeutic targets. These types ofstudies, coupled with published and ongoing studies to lookat message level of specific genes or microarray analysis, areinvaluable tools in the quest to define biological markers ofrenal allograft dysfunction in transplantation.Page 219
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, and several others. In this article, Brinkkoeter et al. examine AngII effects on podocyte production of negatively charged heparan sulfate proteoglycans (HSPG), molecules that constitute a major portion of the negative charge barrier to protein filtration. They find a marked decrease in both cell and matrix HSPG associated with AngII expression. These changes could explain the loss of the charge barrier in proteinuric diseases like diabetic nephropathy, and they also contribute to the reduction of proteinuria seen with AngII inhibitors, which could presumably restore the charge barrier as well as reduce intraglomerular pressure.Page 33 
-5 chain of type IV collagen. The fact that changes similar to those observed in cell culture were also documented in the intact diabetic animal provides strong evidence that the in vitro observations are relevant to what occurs in vivo. While the complex processes that regulate matrix synthesis and degradation in the GBM are certainly more complicated than this, the study does provide novel information on the role of glucose in the pathogenesis of diabetic nephropathy. The next step will be to see if this process can be ameliorated with 12-lipoxygenase inhibitors such as nonsteroidal antiinflammatory agents.Page 112 
