Your search keyword '"Renal Physiology"' showing total 12,476 results

1. HNF1B Transcription Factor: Key Regulator in Renal Physiology and Pathogenesis.

Author

Sánchez-Cazorla, Eloísa, Carrera, Noa, and García-González, Miguel Ángel

Subjects

*MATURITY onset diabetes of the young, *TRANSCRIPTION factors, *KIDNEY physiology, *POLYCYSTIC kidney disease, *GENETIC regulation

Abstract

The HNF1B gene, located on chromosome 17q12, encodes a transcription factor essential for the development of several organs. It regulates the expression of multiple genes in renal, pancreatic, hepatic, neurological, and genitourinary tissues during prenatal and postnatal development, influencing processes such as nephrogenesis, cellular polarity, tight junction formation, cilia development, ion transport in the renal tubule, and renal metabolism. Mutations that alter the function of Hnf1b deregulate those processes, leading to various pathologies characterized by both renal and extrarenal manifestations. The main renal diseases that develop are polycystic kidney disease, hypoplastic or dysplastic kidneys, structural abnormalities, Congenital Anomalies of the Kidney and Urinary Tract (CAKUT), and electrolyte imbalances such as hyperuricemia and hypomagnesemia. Extrarenal manifestations include Maturity-Onset Diabetes of the Young (MODY), hypertransaminasemia, genital and urinary tract malformations, Autism Spectrum Disorder (ASD), and other neurodevelopmental disorders. Patients with HNF1B alterations typically carry either punctual mutations or a monoallelic microdeletion in the 17q12 region. Future research on the molecular mechanisms and genotype–phenotype correlations in HNF1B-related conditions will enhance our understanding, leading to improved clinical management, genetic counseling, monitoring, and patient care. [ABSTRACT FROM AUTHOR]

Published

2024

2. Study preferences and exam outcomes in medical education: insights from renal physiology.

Author

Heltne, Sofie Fagervoll, Hovdenakk, Sigrid, Kvernenes, Monika, and Tenstad, Olav

Subjects

MEDICAL students, KIDNEY physiology, TEACHING methods, ACTIVE learning, EDUCATIONAL outcomes

Abstract

Background: Efficient learning strategies and resource utilization are critical in medical education, especially for complex subjects like renal physiology. This is increasingly important given the rise in chronic renal diseases and the decline in nephrology fellowships. However, the correlations between study time, perceived utility of learning resources, and academic performance are not well-explored, which led to this study. Methods: A cross-sectional survey was conducted with second-year medical students at the University of Bergen, Norway, to assess their preferred learning resources and study time dedicated to renal physiology. Responses were correlated with end-of-term exam scores. Results: The study revealed no significant correlation between time spent studying and overall academic performance, highlighting the importance of study quality over quantity. Preferences for active learning resources, such as Team-Based Learning, interactive lessons and formative assignments, were positively correlated with better academic performance. A notable correlation was found between students' valuation of teachers' professional competence and their total academic scores. Conversely, perceived difficulty across the curriculum and reliance on self-found online resources in renal physiology correlated negatively with academic performance. 'The Renal Pod', a locally produced renal physiology podcast, was popular across grades. Interestingly, students who listened to all episodes once achieved higher exam scores compared to those who listened to only some episodes, reflecting a strategic approach to podcast use. Textbooks, while less popular, did not correlate with higher exam scores. Despite the specific focus on renal physiology, learning preferences are systematically correlated with broader academic outcomes, reflecting the interconnected nature of medical education. Conclusion: The study suggests that the quality and strategic approaches to learning significantly impact academic performance. Successful learners tend to be proactive, engaged, and strategic, valuing expert instruction and active participation. These findings support the integration of student-activating teaching methods and assignments that reward deep learning. [ABSTRACT FROM AUTHOR]

Published

2024

3. Study preferences and exam outcomes in medical education: insights from renal physiology

Author

Sofie Fagervoll Heltne, Sigrid Hovdenakk, Monika Kvernenes, and Olav Tenstad

Subjects

Renal physiology, Teaching methods, Medical school, Learning resources, Academic achievement, Medical students, Special aspects of education, LC8-6691, Medicine

Abstract

Abstract Background Efficient learning strategies and resource utilization are critical in medical education, especially for complex subjects like renal physiology. This is increasingly important given the rise in chronic renal diseases and the decline in nephrology fellowships. However, the correlations between study time, perceived utility of learning resources, and academic performance are not well-explored, which led to this study. Methods A cross-sectional survey was conducted with second-year medical students at the University of Bergen, Norway, to assess their preferred learning resources and study time dedicated to renal physiology. Responses were correlated with end-of-term exam scores. Results The study revealed no significant correlation between time spent studying and overall academic performance, highlighting the importance of study quality over quantity. Preferences for active learning resources, such as Team-Based Learning, interactive lessons and formative assignments, were positively correlated with better academic performance. A notable correlation was found between students’ valuation of teachers’ professional competence and their total academic scores. Conversely, perceived difficulty across the curriculum and reliance on self-found online resources in renal physiology correlated negatively with academic performance. ‘The Renal Pod’, a locally produced renal physiology podcast, was popular across grades. Interestingly, students who listened to all episodes once achieved higher exam scores compared to those who listened to only some episodes, reflecting a strategic approach to podcast use. Textbooks, while less popular, did not correlate with higher exam scores. Despite the specific focus on renal physiology, learning preferences are systematically correlated with broader academic outcomes, reflecting the interconnected nature of medical education. Conclusion The study suggests that the quality and strategic approaches to learning significantly impact academic performance. Successful learners tend to be proactive, engaged, and strategic, valuing expert instruction and active participation. These findings support the integration of student-activating teaching methods and assignments that reward deep learning.

Published

2024

4. Commensal microbiota regulate aldosterone.

Author

Moore, Brittni N., Medcalf, Alexandra D., Muir, Rachel Q., Xu, Chudan, Marques, Francine Z., and Pluznick, Jennifer L.

Subjects

*ALDOSTERONE, *GUT microbiome, *ENZYME-linked immunosorbent assay, *KIDNEY physiology, *BLOOD pressure

Abstract

The gut microbiome regulates many important host physiological processes associated with cardiovascular health and disease; however, the impact of the gut microbiome on aldosterone is unclear. Investigating whether gut microbiota regulate aldosterone can offer novel insights into how the microbiome affects blood pressure. In this study, we aimed to determine whether gut microbiota regulate host aldosterone. We used enzyme-linked immunosorbent assays (ELISAs) to assess plasma aldosterone and plasma renin activity (PRA) in female and male mice in which gut microbiota are intact, suppressed, or absent. In addition, we examined urinary aldosterone. Our findings demonstrated that when the gut microbiota is suppressed following antibiotic treatment, there is an increase in plasma and urinary aldosterone in both female and male mice. In contrast, an increase in PRA is seen only in males. We also found that when gut microbiota are absent (germ-free mice), plasma aldosterone is significantly increased compared with conventional animals (in both females and males), but PRA is not. Understanding how gut microbiota influence aldosterone levels could provide valuable insights into the development and treatment of hypertension and/or primary aldosteronism. This knowledge may open new avenues for therapeutic interventions, such as probiotics or dietary modifications to help regulate blood pressure via microbiota-based changes to aldosterone. NEW & NOTEWORTHY: We explore the role of the gut microbiome in regulating aldosterone, a hormone closely linked to blood pressure and cardiovascular disease. Despite the recognized importance of the gut microbiome in host physiology, the relationship with circulating aldosterone remains largely unexplored. We demonstrate that suppression of gut microbiota leads to increased levels of plasma and urinary aldosterone. These findings underscore the potential of the gut microbiota to influence aldosterone regulation, suggesting new possibilities for treating hypertension. [ABSTRACT FROM AUTHOR]

Published

2024

5. Strategies for Operationalizing Xenotransplantation

Author

Anderson, Douglas J. and Locke, Jayme E.

Published

2024

6. Development of a reference interval for urinary ammonia‐to‐creatinine ratio in feline patients.

Author

Brown, Eleanor E., Castro, Rebecca A., Griffin, Francesca C., Mandese, Wendy W., Rooks, Jenna K., Stone, Amy E., Wuerz, Julia A., Cooke, Kirsten L., Specht, Andrew J., and Harris, Autumn N.

Subjects

VETERINARY clinical pathology, HOMEOSTASIS, BIOCHEMISTRY, KIDNEY physiology, DISEASE progression

Abstract

Background: Disruption of acid–base homeostasis can lead to many clinical problems. Ammonia excretion by the kidneys is critical to maintaining acid–base homeostasis through bicarbonate production. Measurement of ammonia excretion may help determine if the kidneys are properly functioning in maintaining acid–base balance. Reference intervals are essential tools for clinical decision‐making but do not currently exist for urinary ammonia‐to‐creatinine ratio (UACR) in feline patients. Objective: This study aimed to generate a reference interval (RI) for UACR in healthy adult cats. Methods: The study used samples from client‐owned adult healthy cats that presented to the University of Florida Primary Care and Dentistry service (n = 92). Physical examination, serum biochemistry, urinalysis, urine ammonia, and creatinine concentrations were measured. Cats were excluded if there were significant abnormalities in their urinalysis or biochemistry panel. The RI for UACR was calculated according to the recommendation of the American Society for Veterinary Clinical Pathology. The UACR was evaluated for correlation with serum bicarbonate, weight, age, and sex. Results: The RI for UACR was 3.4–20.7 with 90% confidence intervals for the lower and upper limits of (3.0–3.7) and (16.0–23.7), respectively. No significant correlation with age, sex, or weight was found. There was no discernable relationship between serum bicarbonate and UACR. Conclusions: Establishing an RI for UACR in healthy adult cats will allow further studies to determine if changes in UACR are observed during specific disease states. [ABSTRACT FROM AUTHOR]

Published

2024

7. Understanding fluid dynamics and renal perfusion in acute kidney injury management

Author

Messina, Antonio, Calatroni, Marta, Castellani, Gianluca, De Rosa, Silvia, Ostermann, Marlies, and Cecconi, Maurizio

Published

2024

8. Renal System, Fluid Balance, and Its Adaptations to Exercise

Author

Gokcen, Selda, Kaya Utlu, Defne, editor, Sayaca, Cetin, Section Editor, Özkal, Özden, Section Editor, Tayfur, Abdulhamit, Section Editor, Erdem Eyüboğlu, Filiz, Section Editor, and Calik, Mahmut, Section Editor

Published

2023

9. Renal Organic Anion Transporters 1 and 3 In Vitro: Gone but Not Forgotten.

Author

Caetano-Pinto, Pedro and Stahl, Simone H.

Subjects

*ORGANIC anion transporters, *PROXIMAL kidney tubules, *KIDNEY tubules, *SMALL molecules, *ESSENTIAL drugs, *KIDNEY physiology

Abstract

Organic anion transporters 1 and 3 (OAT1 and OAT3) play a crucial role in kidney function by regulating the secretion of multiple renally cleared small molecules and toxic metabolic by-products. Assessing the activity of these transporters is essential for drug development purposes as they can significantly impact drug disposition and safety. OAT1 and OAT3 are amongst the most abundant drug transporters expressed in human renal proximal tubules. However, their expression is lost when cells are isolated and cultured in vitro, which is a persistent issue across all human and animal renal proximal tubule cell models, including primary cells and cell lines. Although it is well known that the overall expression of drug transporters is affected in vitro, the underlying reasons for the loss of OAT1 and OAT3 are still not fully understood. Nonetheless, research into the regulatory mechanisms of these transporters has provided insights into the molecular pathways underlying their expression and activity. In this review, we explore the regulatory mechanisms that govern the expression and activity of OAT1 and OAT3 and investigate the physiological changes that proximal tubule cells undergo and that potentially result in the loss of these transporters. A better understanding of the regulation of these transporters could aid in the development of strategies, such as introducing microfluidic conditions or epigenetic modification inhibitors, to improve their expression and activity in vitro and to create more physiologically relevant models. Consequently, this will enable more accurate assessment for drug development and safety applications. [ABSTRACT FROM AUTHOR]

Published

2023

10. Nanodrugs alleviate acute kidney injury: Manipulate RONS at kidney

Author

Qiaohui Chen, Yayun Nan, Yuqi Yang, Zuoxiu Xiao, Min Liu, Jia Huang, Yuting Xiang, Xingyu Long, Tianjiao Zhao, Xiaoyuan Wang, Qiong Huang, and Kelong Ai

Subjects

Reactive oxygen and nitrogen species, Acute kidney injury, Nanomaterials, Antioxidant therapy, Renal physiology, Materials of engineering and construction. Mechanics of materials, TA401-492, Biology (General), QH301-705.5

Abstract

Currently, there are no clinical drugs available to treat acute kidney injury (AKI). Given the high prevalence and high mortality rate of AKI, the development of drugs to effectively treat AKI is a huge unmet medical need and a research hotspot. Although existing evidence fully demonstrates that reactive oxygen and nitrogen species (RONS) burst at the AKI site is a major contributor to AKI progression, the heterogeneity, complexity, and unique physiological structure of the kidney make most antioxidant and anti-inflammatory small molecule drugs ineffective because of the lack of kidney targeting and side effects. Recently, nanodrugs with intrinsic kidney targeting through the control of size, shape, and surface properties have opened exciting prospects for the treatment of AKI. Many antioxidant nanodrugs have emerged to address the limitations of current AKI treatments. In this review, we systematically summarized for the first time about the emerging nanodrugs that exploit the pathological and physiological features of the kidney to overcome the limitations of traditional small-molecule drugs to achieve high AKI efficacy. First, we analyzed the pathological structural characteristics of AKI and the main pathological mechanism of AKI: hypoxia, harmful substance accumulation-induced RONS burst at the renal site despite the multifactorial initiation and heterogeneity of AKI. Subsequently, we introduced the strategies used to improve renal targeting and reviewed advances of nanodrugs for AKI: nano-RONS-sacrificial agents, antioxidant nanozymes, and nanocarriers for antioxidants and anti-inflammatory drugs. These nanodrugs have demonstrated excellent therapeutic effects, such as greatly reducing oxidative stress damage, restoring renal function, and low side effects. Finally, we discussed the challenges and future directions for translating nanodrugs into clinical AKI treatment.

Published

2023

11. A proline‐tyrosine motif, endocytosis and low salt – how to link protein functions to organ physiology.

Author

Fahlke, Christoph

Subjects

*CHLORIDE channels, *GENETIC mutation, *PROTEIN expression, *ENDOCYTOSIS, *XENOPUS, *PHYSIOLOGY

Abstract

The author comments on a study that demonstrates how a mutation in the anion chloride channel ClC-K-barttin affects an endocytic YxxØ motif and uses expression in Xenopus oocytes and mammalian cells to link increased stability of the ClC-K-barttin complex. He discusses the finding that the barttin point mutation left protein expression levels and subcellular distribution unaffected under control conditions. He explains the significance of linking protein functions to organ physiology.

Published

2024

12. Editorial: Proteomics, mass spectrometry and bioinformatics in renal pathophysiology

Author

Timothy D. Cummins and Visith Thongboonkerd

Subjects

bioinformatics, biomarker, mass spectrometry, proteomics, renal pathology, renal physiology, Physiology, QP1-981

Published

2023

13. Designing and Reflecting on Active Learning and Flipped Classrooms for Renal Physiology

Author

Bernard Thomas Drumm

Subjects

flipped classes, renal physiology, active learning, classroom assessment, Theory and practice of education, LB5-3640

Abstract

In this paper, we outline a case study describing the incorporation of active learning and flipped classroom techniques in a renal physiology module in 1st year medical school. The module was redesigned over a 2-year period within the teaching for understanding (TfU) framework (generative topics, understanding goals, performances of understanding and ongoing assessment) to include more active learning exercises (clicker response systems centered on clinically relevant problem sets and classroom assessment techniques – CATs), which culminated in flipping the classroom entirely during the 2nd year. The goal, was to evaluate student perceptions of the flipped classroom model and to reflect on the use of active learning generally. In the 1st year, clicker response systems were favorably received by students, however the anonymous nature of the clicker configuration meant it was not possible to track progress of individual students. CATs revealed that content areas without active learning exercises were often deemed the most unclear by students. Student feedback indicated that the flipped classroom model in the 2nd year was positively received, with students noting it encouraged them to attend classes more regularly and they believed it assisted in developing collaborative learning and knowledge application.

Published

2023

14. Renal Regulation of Acid-Base Metabolism

Author

Muñoz, Ricardo and Muñoz, Ricardo, editor

Published

2022

15. Role of FXR in Renal Physiology and Kidney Diseases.

Author

Guo, Yanlin, Xie, Guixiang, and Zhang, Xiaoyan

Subjects

*FARNESOID X receptor, *KIDNEY physiology, *KIDNEY diseases, *DIABETIC nephropathies, *CHRONIC kidney failure, *ADRENAL glands

Abstract

Farnesoid X receptor, also known as the bile acid receptor, belongs to the nuclear receptor (NR) superfamily of ligand-regulated transcription factors, which performs its functions by regulating the transcription of target genes. FXR is highly expressed in the liver, small intestine, kidney and adrenal gland, maintaining homeostasis of bile acid, glucose and lipids by regulating a diverse array of target genes. It also participates in several pathophysiological processes, such as inflammation, immune responses and fibrosis. The kidney is a key organ that manages water and solute homeostasis for the whole body, and kidney injury or dysfunction is associated with high morbidity and mortality. In the kidney, FXR plays an important role in renal water reabsorption and is thought to perform protective functions in acute kidney disease and chronic kidney disease, especially diabetic kidney disease. In this review, we summarize the recent advances in the understanding of the physiological and pathophysiological function of FXR in the kidney. [ABSTRACT FROM AUTHOR]

Published

2023

16. Magnetic resonance imaging during warm ex vivo kidney perfusion.

Author

Schutter, Rianne, van Varsseveld, Otis C., Lantinga, Veerle A., Pool, Merel B. F., Hamelink, Tim H., Potze, Jan Hendrik, Leuvenink, Henri G. D., Laustsen, Christoffer, Borra, Ronald J. H., and Moers, Cyril

Subjects

*MAGNETIC resonance imaging, *PERFUSION, *KIDNEY physiology, *KIDNEYS, *CELLULAR therapy, *TRANSPLANTATION of organs, tissues, etc.

Abstract

Background: The shortage of donor organs for transplantation remains a worldwide problem. The utilization of suboptimal deceased donors enlarges the pool of potential organs, yet consequently, clinicians face the difficult decision of whether these sub‐optimal organs are of sufficient quality for transplantation. Novel technologies could play a pivotal role in making pre‐transplant organ assessment more objective and reliable. Methods: Ex vivo normothermic machine perfusion (NMP) at temperatures around 35–37°C allows organ quality assessment in a near‐physiological environment. Advanced magnetic resonance imaging (MRI) techniques convey unique information about an organ's structural and functional integrity. The concept of applying magnetic resonance imaging during renal normothermic machine perfusion is novel in both renal and radiological research and we have developed the first MRI‐compatible NMP setup for human‐sized kidneys. Results: We were able to obtain a detailed and real‐time view of ongoing processes inside renal grafts during ex vivo perfusion. This new technique can visualize structural abnormalities, quantify regional flow distribution, renal metabolism, and local oxygen availability, and track the distribution of ex vivo administered cellular therapy. Conclusion: This platform allows for advanced pre‐transplant organ assessment, provides a new realistic tool for studies into renal physiology and metabolism, and may facilitate therapeutic tracing of pharmacological and cellular interventions to an isolated kidney. [ABSTRACT FROM AUTHOR]

Published

2023

17. NOXA1-dependent NADPH oxidase 1 signaling mediates angiotensin II activation of the epithelial sodium channel.

Author

Mironova, Elena, Archer, Crystal R., Vendrov, Aleksandr E., Runge, Marschall S., Madamanchi, Nageswara R., Arendshorst, William J., Stockand, James D., and Abd El-Aziz, Tarek Mohamed

Subjects

*ANGIOTENSIN II, *NADPH oxidase, *SODIUM channels, *RENIN-angiotensin system, *BLOOD pressure, *CELL membranes

Abstract

The activity of the epithelial Na+ channel (ENaC) in principal cells of the distal nephron fine-tunes renal Na+ excretion. The renin-angiotensin-aldosterone system modulates ENaC activity to control blood pressure, in part, by influencing Na+ excretion. NADPH oxidase activator 1-dependent NADPH oxidase 1 (NOXA1/NOX1) signaling may play a key role in angiotensin II (ANG II)- dependent activation of ENaC. The present study aimed to explore the role of NOXA1/NOX1 signaling in ANG II-dependent activation of ENaC in renal principal cells. Patch-clamp electrophysiology and principal cell-specific Noxa1 knockout (PC-Noxa1 KO) mice were used to determine the role of NOXA1/NOX1 signaling in ANG II-dependent activation of ENaC. The activity of ENaC in the luminal plasma membrane of principal cells was quantified in freshly isolated split-opened tubules using voltage-clamp electrophysiology. ANG II significantly increased ENaC activity. This effect was robust and observed in response to both acute (40 min) and more chronic (48–72 h) ANG II treatment of isolated tubules and mice, respectively. Inhibition of ANG II type 1 receptors with losartan abolished ANG II-dependent stimulation of ENaC. Similarly, treatment with ML171, a specific inhibitor of NOX1, abolished stimulation of ENaC by ANG II. Treatment with ANG II failed to increase ENaC activity in principal cells in tubules isolated from the PC-Noxa1 KO mouse. Tubules from wild-type littermate controls, though, retained their ability to respond to ANG II with an increase in ENaC activity. These results indicate that NOXA1/NOX1 signaling mediates ANG II stimulation of ENaC in renal principal cells. As such, NOXA1/NOX1 signaling in the distal nephron plays a central role in Na+ homeostasis and control of blood pressure, particularly as it relates to regulation by the renin-ANG II axis. NEW & NOTEWORTHY Activity of the epithelial Na+ channel (ENaC) in the distal nephron fine-tunes renal Na+ excretion. Angiotensin II (ANG II) has been reported to enhance ENaC activity. Emerging evidence suggests that NADPH oxidase (NOX) signaling plays an important role in the stimulation of ENaC by ANG II in principal cells. The present findings indicate that NOX activator 1/NOX1 signaling mediates ANG II stimulation of ENaC in renal principal cells. [ABSTRACT FROM AUTHOR]

Published

2022

18. SGLT2 inhibition and kidney protection.

Author

Nespoux, Josselin and Vallon, Volker

Subjects

Kidney Disease, Diabetes, Cardiovascular, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Renal and urogenital, Metabolic and endocrine, Good Health and Well Being, Acute Kidney Injury, Biological Transport, Active, Blood Glucose, Blood Pressure, Diabetes Mellitus, Type 2, Diabetic Nephropathies, Glomerular Filtration Rate, Heart Failure, Humans, Hypoglycemic Agents, Kidney, Sodium-Glucose Transporter 2 Inhibitors, diabetic nephropathy, glucose transport, renal physiology, Medical and Health Sciences, Cardiovascular System & Hematology

Abstract

Type 2 diabetes mellitus (T2DM) is a growing public health concern worldwide. Numerous drug classes are available for treatment, however, their efficacy with regard to diabetes-induced renal and cardiovascular (CV) complications remains limited. Inhibitors of the sodium-glucose cotransporter 2 (SGLT2) are a new class of blood glucose lowering medications that block renal glucose reabsorption and have protective effects on the kidney and the heart. This review focusses on the effects of SGLT2 inhibitors on the kidney and renal outcome: it briefly outlines renal glucose handling in diabetes and its role in glomerular hyperfiltration and renal hypoxia; describes how SGLT2 inhibitors induce an early, reversible reduction in glomerular filtration rate (GFR) and preserve GFR in the long-term in patients with T2DM; discusses whether the enhanced active transport in the renal outer medulla (OM) in response to SGLT2 inhibition is friend or foe; proposes how the blood pressure lowering and heart failure protective effect of SGLT2 inhibitors can be preserved in chronic kidney disease (CKD) despite attenuated antihyperglycemic effects; and examines whether SGLT2 inhibition enhances the incidence or severity of acute kidney injury (AKI).

Published

2018

19. Evolving Concepts in Uromodulin Biology, Physiology, and Its Role in Disease: a Tale of Two Forms.

Author

LaFavers, Kaice A., Micanovic, Radmila, Sabo, Angela R., Maghak, Lauren A., and El-Achkar, Tarek M.

Abstract

Uromodulin (or Tamm-Horsfall protein) is a glycoprotein uniquely produced in the kidney by tubular cells of the thick ascending limb of the loop of Henle and early distal tubules. This protein exhibits bidirectional secretion in the urine and in the renal interstitium and circulation. The role of this protein in maintaining renal and systemic homeostasis is becoming increasingly appreciated. Furthermore, perturbations of its functions may play a role in various diseases affecting the kidney and distant organs. In this review, we will discuss important advances in understanding its biology, highlighting the recent discoveries of its secretion and differential precursor processing that generates 2 forms: (1) a highly polymerizing form that is apically excreted in the urine and generates filaments and (2) a nonpolymerizing form that retains a polymerization inhibitory pro-peptide and is released basolaterally in the kidney interstitium and circulation, but can also be found in the urine. We will also discuss factors regulating its production and release, taking into account its intricate physiology, and propose best practices to report its levels. We also discuss breaking advances in its role in hypertension, acute kidney injury and progression to chronic disease, immunomodulation and regulating renal and systemic oxidative stress. We anticipate that this work will be a great resource for researchers and clinicians. This review will highlight the importance of defining what regulates the 2 forms of uromodulin, so that modulation of uromodulin levels and function could become a novel tool in our therapeutic armamentarium against kidney disease. [ABSTRACT FROM AUTHOR]

Published

2022

20. Renal Corin Is Essential for Normal Blood Pressure and Sodium Homeostasis.

Author

Zhou, Tiantian, Zhang, Shengnan, Du, Chunyu, Wang, Kun, Gu, Xiabing, Sun, Shijin, Zhang, Xianrui, Niu, Yayan, Wang, Can, Liu, Meng, Dong, Ningzheng, and Wu, Qingyu

Subjects

*ATRIAL natriuretic peptides, *HOMEOSTASIS, *HIGH-salt diet, *KIDNEY physiology, *SODIUM

Abstract

Atrial natriuretic peptide (ANP)-mediated natriuresis is known as a cardiac endocrine function in sodium and body fluid homeostasis. Corin is a protease essential for ANP activation. Here, we studied the role of renal corin in regulating salt excretion and blood pressure. We created corin conditional knockout (cKO), in which the Corin gene was selectively disrupted in the kidney (kcKO) or heart (hcKO). We examined the blood pressure, urinary Na+ and Cl− excretion, and cardiac hypertrophy in wild-type, corin global KO, kcKO, and hcKO mice fed normal- and high-salt diets. We found that on a normal-salt diet (0.3% NaCl), corin kcKO and hcKO mice had increased blood pressure, indicating that both renal and cardiac corin is necessary for normal blood pressure in mice. On a high-salt diet (4% NaCl), reduced urinary Na+ and Cl− excretion, increased body weight, salt-exacerbated hypertension, and cardiac hypertrophy were observed in corin kcKO mice. In contrast, impaired urinary Na+ and Cl− excretion and salt-exacerbated hypertension were not observed in corin hcKO mice. These results indicated that renal corin function is important in enhancing natriuresis upon high salt intakes and that this function cannot be compensated by the cardiac corin function in mice. [ABSTRACT FROM AUTHOR]

Published

2022

21. The Effects of Targeted Changes in Systemic Blood Flow and Mean Arterial Pressure on Urine Oximetry During Cardiopulmonary Bypass.

Author

Hu, Raymond, Yanase, Fumitaka, McCall, Peter, Evans, Roger, Raman, Jaishankar, and Bellomo, Rinaldo

Abstract

Poor medullary oxygenation is implicated in the evolution of acute kidney injury. The authors sought to determine if increasing systemic flow and mean arterial pressure could improve urine oxygen tension (PuO 2) measured in the bladder, a surrogate of kidney medullary oxygenation, in patients undergoing on-pump cardiac surgery. Randomized crossover study. University-affiliated hospital. Twenty adult patients undergoing cardiopulmonary bypass (CPB) with expected cross-clamp time of >60 minutes and estimated glomerular filtration rate of >30 mL/min/1.73m2. Sequential 20-minute periods of 2 interventions: Intervention H ("High") or Intervention N ("Normal"). The order of interventions was determined by randomization. Intervention H: targeted CPB flow 3.0 L/min/m2 and mean arterial pressure (MAP) 80 mmHg. Intervention N: targeted CPB flow 2.4 L/min/m2 and MAP 65 mmHg. PuO 2 was measured by an oxygen sensor introduced into the bladder via a urinary catheter. Clear separation was achieved in CPB flow and MAP between intervention periods (p < 0.001 for group-time interaction). PuO 2 during Intervention H was higher than during Intervention N (p < 0.001 for group-time interaction). After 17 minutes, PuO 2 was statistically higher in Intervention H at each time point. There were no differences in markers of hemolysis between interventions. PuO 2 was higher when systemic flow and MAP were increased during CPB. These findings suggest that PuO 2 is responsive to changes in hemodynamics and that higher flow and pressure may improve medullary oxygenation. [ABSTRACT FROM AUTHOR]

Published

2022

22. Dr. Manuel Martinez-Maldonado: A Pioneer in Renal Therapeutics and Mentor to a Generation of Minority Physician-Scientists.

Author

Figueroa-Quintana JR, Rajput S, Chow DJ, and Estapé ES

Abstract

Dr. Manuel Martinez-Maldonado is a distinguished Puerto Rican internist, nephrologist, physician-scientist, mentor, and prolific writer whose leadership in academic and clinical settings has significantly advanced the fields of nephrology, renal physiology and pharmacology, fluids and electrolyte metabolism, calcium metabolism, hypertension research, and medical education. His research on electrolyte imbalances has led to innovative hypercalcemia treatments, notably furosemide with IV fluid therapy. This is an approach that, combined with pharmacotherapy using calcitonin and bisphosphonates, became the standard practice for managing hypercalcemia until specific therapies became available. His nephrology research team and laboratory in the San Juan VA (Veterans Affairs) Medical Center and the Medical School of the University of Puerto Rico were internationally renowned. Throughout his career, he fostered a culture of mentorship while spearheading superb clinical teaching and research initiatives. His transformative tenures at several institutions, including Baylor College of Medicine; the University of Puerto Rico-Medical Sciences Campus; the VA medical centers in Atlanta, Houston, and San Juan; Emory University; Oregon Health Sciences University; Ponce School of Medicine; and the University of Louisville School of Medicine demonstrate his lasting contributions to medical science and education. His interdisciplinary approach, advocacy for kidney and clinical research, and contributions to understanding the renin-angiotensin system and the role of sodium-potassium-activated adenosine triphosphatase in renal concentration mechanisms illustrate his enduring impact on renal physiology and human health., Competing Interests: Conflicts of interest: In compliance with the ICMJE uniform disclosure form, all authors declare the following: Payment/services info: All authors have declared that no financial support was received from any organization for the submitted work. Financial relationships: All authors have declared that they have no financial relationships at present or within the previous three years with any organizations that might have an interest in the submitted work. Other relationships: All authors have declared that there are no other relationships or activities that could appear to have influenced the submitted work., (Copyright © 2024, Figueroa-Quintana et al.)

Published

2024

23. The European and Japanese eel NaCl cotransporters β exhibit chloride currents and are resistant to thiazide type diuretics.

Author

Moreno, Erika, Plata, Consuelo, Vázquez, Norma, María Oropeza-Viveros, Dulce, Pacheco-Alvarez, Diana, Rojas-Vega, Lorena, Olin-Sandova, Viridiana, and Gamba, Gerardo

Subjects

*ANGUILLA japonica, *ANGUILLA anguilla, *SALT, *DIURETICS, *CHLORIDES, *CHLORIDE ions

Abstract

The thiazide-sensitive Na+-Cl- cotransporter (NCC) is the major pathway for salt reabsorption in the mammalian distal convoluted tubule, and the inhibition of its function with thiazides is widely used for the treatment of arterial hypertension. In mammals and teleosts, NCC is present as one ortholog that is mainly expressed in the kidney. One exception, however, is the eel, which has two genes encoding NCC. The eNCCα is located in the kidney and eNCCβ, which is present in the apical membrane of the rectum. Interestingly, the European eNCCβ functions as a Na+-Cl- cotransporter that is nevertheless resistant to thiazides and is not activated by low-chloride hypotonic stress. However, in the Japanese eel rectal sac, a thiazide-sensitive NaCl transport mechanism has been described. The protein sequences between eNCCβ and jNCCβ are 98% identical. Here, by site-directed mutagenesis, we transformed eNCCβ into jNCCβ. Our data showed that jNCCβ, similar to eNCCβ, is resistant to thiazides. In addition, both NCCβ proteins have high transport capacity with respect to their renal NCC orthologs and, in contrast to known NCCs, exhibit electrogenic properties that are reduced when residue I172 is substituted by A, G, or M. This is considered a key residue for the chloride ion-binding sites of NKCC and KCC. We conclude that NCCβ proteins are not sensitive to thiazides and have electrogenic properties dependent on Cl-, and site I172 is important for the function of NCCβ. [ABSTRACT FROM AUTHOR]

Published

2022

24. Findings from Clinical University Hospital in Transcription Factors Reported (HNF1B Transcription Factor: Key Regulator in Renal Physiology and Pathogenesis).

Abstract

Researchers at the Clinical University Hospital in Santiago de Compostela, Spain, have identified the HNF1B gene as a key regulator in renal physiology and pathogenesis. This gene encodes a transcription factor that plays a crucial role in the development of various organs, including the kidneys. Mutations in HNF1B can lead to a range of renal and extrarenal manifestations, such as polycystic kidney disease, Maturity-Onset Diabetes of the Young (MODY), and neurodevelopmental disorders. Further research on the molecular mechanisms and genotype-phenotype correlations of HNF1B-related conditions is needed to enhance clinical management and patient care. [Extracted from the article]

Published

2024

25. Data on Health and Medicine Described by Researchers at University of Bergen (Study preferences and exam outcomes in medical education: insights from renal physiology).

Abstract

A study conducted at the University of Bergen in Norway explored the relationship between study preferences, learning resources, and academic performance in medical education, specifically focusing on renal physiology. The study found that the quality and strategic approach to learning had a significant impact on academic performance, with active learning resources and engagement correlating positively with better exam scores. The study also highlighted the importance of expert instruction and valuing teachers' professional competence. These findings suggest the integration of student-activating teaching methods and assignments that reward deep learning in medical education. [Extracted from the article]

Published

2024

26. Sex Differences in Renal Function: Participation of Gonadal Hormones and Prolactin

Author

Adriana Franco-Acevedo, Raquel Echavarria, and Zesergio Melo

Subjects

kidney, renal physiology, gender, hormones, prolactin, vasoinhibins, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Kidney pathophysiology is influenced by gender. Evidence suggests that kidney damage is more severe in males than in females and that sexual hormones contribute to this. Elevated prolactin concentration is common in renal impairment patients and is associated with an unfavorable prognosis. However, PRL is involved in the osmoregulatory process and promotes endothelial proliferation, dilatation, and permeability in blood vessels. Several proteinases cleavage its structure, forming vasoinhibins. These fragments have antagonistic PRL effects on endothelium and might be associated with renal endothelial dysfunction, but its role in the kidneys has not been enough investigated. Therefore, the purpose of this review is to describe the influence of sexual dimorphism and gonadal hormones on kidney damage, emphasizing the role of the hormone prolactin and its cleavage products, the vasoinhibins.

Published

2021

27. From Proteinuria to Fibrosis: An Update on Pathophysiology and Treatment Options

Author

Sonia Sharma and Brendan Smyth

Subjects

proteinuria, renal physiology, kidney fibrosis, albuminuria, chronic kidney disease, Dermatology, RL1-803, Diseases of the circulatory (Cardiovascular) system, RC666-701, Diseases of the genitourinary system. Urology, RC870-923

Abstract

Background: Proteinuria is a key biomarker in nephrology. It is central to diagnosis and risk assessment and the primary target of many important therapies. Etiologies resulting in pathological proteinuria include congenital and acquired disorders, as well as both glomerular (immune/non-immune mediated) and tubular defects. Summary: Untreated proteinuria is strongly linked to progressive loss of kidney function and kidney failure. Excess protein reaching the renal tubules is ordinarily resorbed by the tubular epithelium. However, when these mechanisms are overwhelmed, a variety of inflammatory and fibrotic pathways are activated, causing both interstitial fibrosis and glomerulosclerosis. Nevertheless, the specific mechanisms underlying this are complex and remain incompletely understood. Recently, a number of treatments, in addition to angiotensin system blockade, have been shown to effectively slow the progression of proteinuric chronic kidney disease. However, additional therapies are clearly needed. Key message: This review provides an update on the pathophysiology of proteinuria, the pathways leading to fibrosis, and an overview of current and emerging therapies.

Published

2021

28. The drug transporter OAT3 (SLC22A8) and endogenous metabolite communication via the gut–liver–kidney axis

Author

Bush, Kevin T, Wu, Wei, Lun, Christina, and Nigam, Sanjay K

Subjects

Medical Biochemistry and Metabolomics, Biomedical and Clinical Sciences, Chemical Sciences, Digestive Diseases, Kidney Disease, Liver Disease, Oral and gastrointestinal, Amino Acids, Animals, Bile Acids and Salts, Diet, Energy Metabolism, Gastrointestinal Microbiome, Gene Knockout Techniques, Intestinal Mucosa, Intestines, Kidney, Ligands, Lipid Metabolism, Liver, Male, Metabolomics, Mice, Mice, Inbred C57BL, Organic Anion Transport Protein 1, Organic Anion Transporters, Sodium-Independent, Substrate Specificity, Xenobiotics, OAT3, drug transport, kidney, kidney drug transport, multidrug transporter, organic anion, renal physiology, solute carrier, uremic toxin, xenobiotic, Biological Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences

Abstract

The organic anion transporters OAT1 (SLC22A6) and OAT3 (SLC22A8) have similar substrate specificity for drugs, but it is far from clear whether this holds for endogenous substrates. By analysis of more than 600 metabolites in the Oat3KO (Oat3 knockout) by LC/MS, we demonstrate OAT3 involvement in the movement of gut microbiome products, key metabolites, and signaling molecules, including those flowing through the gut-liver-kidney axis. Major pathways affected included those involved in metabolism of bile acids, flavonoids, nutrients, amino acids (including tryptophan-derivatives that are uremic toxins), and lipids. OAT3 is also critical in elimination of liver-derived phase II metabolites, particularly those undergoing glucuronidation. Analysis of physicochemical features revealed nine distinct metabolite groups; at least one member of most clusters has been previously validated in transport assays. In contrast to drugs interacting with the OATs, endogenous metabolites accumulating in the Oat1KO (Oat1 knockout) versus Oat3KO have distinct differences in their physicochemical properties; they are very different in size, number of rings, hydrophobicity, and molecular complexity. Consistent with the Remote Sensing and Signaling Hypothesis, the data support the importance of the OAT transporters in inter-organ and inter-organismal remote communication via transporter-mediated movement of key metabolites and signaling molecules (e.g. gut microbiome-to-intestine-to-blood-to-liver-to-kidney-to-urine). We discuss the possibility of an intimate connection between OATs and metabolite sensing and signaling pathways (e.g. bile acids). Furthermore, the metabolomics and pathway analysis support the view that OAT1 plays a greater role in kidney proximal tubule metabolism and OAT3 appears relatively more important in systemic metabolism, modulating levels of metabolites flowing through intestine, liver, and kidney.

Published

2017

29. Intravital Imaging with Two-Photon Microscopy: A Look into the Kidney.

Author

Costanzo, Vincenzo and Costanzo, Michele

Subjects

MICROSCOPY, KIDNEY physiology, CELL imaging, FLUORESCENT dyes, FLUORESCENCE microscopy, KIDNEYS

Abstract

Fluorescence microscopy has represented a crucial technique to explore the cellular and molecular mechanisms in the field of biomedicine. However, the conventional one-photon microscopy exhibits many limitations when living samples are imaged. The new technologies, including two-photon microscopy (2PM), have considerably improved the in vivo study of pathophysiological processes, allowing the investigators to overcome the limits displayed by previous techniques. 2PM enables the real-time intravital imaging of the biological functions in different organs at cellular and subcellular resolution thanks to its improved laser penetration and less phototoxicity. The development of more sensitive detectors and long-wavelength fluorescent dyes as well as the implementation of semi-automatic software for data analysis allowed to gain insights in essential physiological functions, expanding the frontiers of cellular and molecular imaging. The future applications of 2PM are promising to push the intravital microscopy beyond the existing limits. In this review, we provide an overview of the current state-of-the-art methods of intravital microscopy, focusing on the most recent applications of 2PM in kidney physiology. [ABSTRACT FROM AUTHOR]

Published

2022

30. Establishment of an RI for the urine ammonia‐to‐creatinine ratio in dogs.

Author

Adrianowycz, Sarah E., Castro, Rebeca A., Specht, Andrew J., and Harris, Autumn N.

Subjects

VETERINARY clinical pathology, DOGS, ACID-base imbalances, URINE, KIDNEY physiology

Abstract

Background: Ammonia is produced and excreted by the kidney, contributing to systemic acid‐base homeostasis through the production of bicarbonate. Disorders of acid‐base balance can lead to many clinical problems and measuring ammonia excretion helps in determining if the kidneys are responding to acid‐base challenges appropriately. Reference intervals are integral to clinical decision‐making, and there is no current RI for the urine ammonia‐to‐creatinine ratio (UACR) in dogs. Objective: This study aimed to generate an RI for the UACR in healthy adult dogs. Methods: The study used adult, client‐owned dogs that were presented to the University of Florida Primary Care and Dentistry service (n = 60). Physical examinations were performed and serum chemistry and urinalysis samples were obtained. Urine ammonia and creatinine concentrations were determined. Dogs were excluded if there were significant abnormalities in either their urinalysis or serum chemistry results. The RI for the UACR was calculated according to the recommendation of the American Society for Veterinary Clinical Pathology. Data were evaluated for correlation with serum bicarbonate, weight, age, and sex. Results: The RIs for the UACR were 0.16‐23.69 with 90% confidence intervals for the lower and upper limits of (0.13‐1.17) and (20.50‐23.75), respectively. No significant impact of age, sex, or weight was found. There was no discernable relationship between serum bicarbonate and UACR. Conclusions: Establishing an RI for UACR in healthy adult dogs will allow for further studies to determine if alterations are observed during specific disease states. [ABSTRACT FROM AUTHOR]

Published

2021

31. Renal Functional Reserve in Naïve HIV Patients.

Author

Musso CG, Juarez R, Belloso W, Gonzalez-Torres H, Capotondo M, Sergio T, Cristiano F, and Aroca Martinez G

Subjects

Humans, Prospective Studies, Male, Adult, Female, Middle Aged, Kidney physiopathology, Creatinine blood, Cimetidine therapeutic use, Glomerular Filtration Rate, HIV Infections drug therapy, HIV Infections complications, HIV Infections physiopathology

Abstract

Introduction. Renal functional reserve (RFR) is the kidney capability of increasing its basal glomerular filtration rate (GFR) at least 20% after an adequate stimulus. Renal disorders have been reported in seropositive HIV patients, particularly the decrease in glomerular filtration rate (eGFR), nephrotic syndrome, and proximal tubular deficiency associated with the disease itself or the use of some anti-retroviral treatments. Thus, it was decided to carry out a prospective study in order to evaluate if RFR test was preserved in naive HIV patients. Material and Method. GFR was measured by using cimetidine-aided creatinine clearance (CACC), and RFR as described Hellerstein et al. in seropositive naive HIV patients and healthy volunteers. Results. RFR was evaluated in 12 naïve HIV patients who showed positive RFR (24.8±2%), but significantly lower compared to RFR in 9 control individuals (90.3 ± 5%). Conclusion. In this study was found that renal functional reserve was positive in naïve HIV patients, but significantly lower compared to renal functional reserve achieved by seronegative healthy individuals., (Copyright by Società Italiana di Nefrologia SIN, Rome,Italy.)

Published

2024

32. Interventions for renal artery stenosis: Appraisal of novel physiological insights and procedural techniques to improve clinical outcome.

Author

Drieghe B, De Buyzere M, Bové T, and De Backer T

Subjects

Humans, Treatment Outcome, Risk Factors, Renal Artery physiopathology, Renal Artery diagnostic imaging, Endovascular Procedures adverse effects, Endovascular Procedures instrumentation, Patient Selection, Clinical Decision-Making, Renal Artery Obstruction physiopathology, Renal Artery Obstruction therapy, Renal Artery Obstruction diagnostic imaging, Renal Artery Obstruction etiology, Stents

Abstract

Randomized clinical trials failed to show additional benefit of renal artery stenting on top of medical therapy. Instead of writing an obituary on renal artery stenting, we try to explain these disappointing results. A transstenotic pressure gradient is needed to reduce renal perfusion and to activate the renin-angiotensin-aldosterone system. In only a minority of patients included in trials, a transstenotic pressure gradient is measured and reported. Like the coronary circulation, integration of physiological lesion assessment will allow to avoid stenting of non-significant lesions and select those patients that are most likely to benefit from renal artery stenting. Renal artery interventions are associated with peri-procedural complications. Contemporary techniques, including radial artery access, no-touch technique to engage the renal ostium and the use of embolic protection devices, will minimize procedural risk. Combining optimal patient selection and meticulous technique might lead to a netto clinical benefit when renal artery stenting is added to optimal medical therapy., (© 2024 Wiley Periodicals LLC.)

Published

2024

33. Disease-associated missense mutations in the pore loop of polycystin-2 alter its ion channel function in a heterologous expression system.

Author

Staudner T, Geiges L, Khamseekaew J, Sure F, Korbmacher C, and Ilyaskin AV

Subjects

Animals, Humans, Sodium metabolism, Polycystic Kidney, Autosomal Dominant genetics, Polycystic Kidney, Autosomal Dominant metabolism, Polycystic Kidney, Autosomal Dominant pathology, Oocytes metabolism, Mutation, Missense, TRPP Cation Channels genetics, TRPP Cation Channels metabolism, TRPP Cation Channels chemistry, Xenopus laevis

Abstract

Polycystin-2 (PC2) is mutated in ∼15% of patients with autosomal dominant polycystic kidney disease (ADPKD). PC2 belongs to the family of transient receptor potential (TRP) channels and can function as a homotetramer. We investigated whether three disease-associated mutations (F629S, C632R, or R638C) localized in the channel's pore loop alter ion channel properties of human PC2 expressed in Xenopus laevis oocytes. Expression of wild-type (WT) PC2 typically resulted in small but measurable Na + inward currents in the absence of extracellular divalent cations. These currents were no longer observed when individual pore mutations were introduced in WT PC2. Similarly, Na + inward currents mediated by the F604P gain-of-function (GOF) PC2 construct (PC2 F604P) were abolished by each of the three pore mutations. In contrast, when the mutations were introduced in another GOF construct, PC2 L677A N681A, only C632R had a complete loss-of-function effect, whereas significant residual Na + inward currents were observed with F629S (∼15%) and R638C (∼30%). Importantly, the R638C mutation also abolished the Ca 2+ permeability of PC2 L677A N681A and altered its monovalent cation selectivity. To elucidate the molecular mechanisms by which the R638C mutation affects channel function, molecular dynamics (MD) simulations were used in combination with functional experiments and site-directed mutagenesis. Our findings suggest that R638C stabilizes ionic interactions between Na + ions and the selectivity filter residue D643. This probably explains the reduced monovalent cation conductance of the mutant channel. In summary, our data support the concept that altered ion channel properties of PC2 contribute to the pathogenesis of ADPKD., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

34. Differential changes in end organ immune cells and inflammation in salt-sensitive hypertension: effects of lowering blood pressure.

Author

Navaneethabalakrishnan S, Goodlett BL, Smith HL, Cardenas A, Burns A, and Mitchell BM

Subjects

Animals, Male, Female, Lymphangiogenesis drug effects, Antihypertensive Agents pharmacology, Mice, Hydralazine pharmacology, NG-Nitroarginine Methyl Ester pharmacology, Disease Models, Animal, Gonads drug effects, Hypertension immunology, Hypertension physiopathology, Hypertension drug therapy, Hypertension chemically induced, Mice, Inbred C57BL, Blood Pressure drug effects, Sodium Chloride, Dietary adverse effects, Kidney immunology, Kidney drug effects, Inflammation immunology

Abstract

We reported that salt-sensitive hypertension (SSHTN) is associated with increased pro-inflammatory immune cells, inflammation, and inflammation-associated lymphangiogenesis in the kidneys and gonads of male and female mice. However, it is unknown whether these adverse end organ effects result from increased blood pressure (BP), elevated levels of salt, or both. We hypothesized that pharmaceutically lowering BP would not fully alleviate the renal and gonadal immune cell accumulation, inflammation, and lymphangiogenesis associated with SSHTN. SSHTN was induced in male and female C57BL6/J mice by administering nitro-L-arginine methyl ester hydrochloride (L-NAME; 0.5 mg/ml) in their drinking water for 2 weeks, followed by a 2-week washout period. Subsequently, the mice received a 3-week 4% high salt diet (SSHTN). The treatment group underwent the same SSHTN induction protocol but received hydralazine (HYD; 250 mg/L) in their drinking water during the diet phase (SSHTN+HYD). Control mice received tap water and a standard diet for 7 weeks. In addition to decreasing systolic BP, HYD treatment generally decreased pro-inflammatory immune cells and inflammation in the kidneys and gonads of SSHTN mice. Furthermore, the decrease in BP partially alleviated elevated renal and gonadal lymphatics and improved renal and gonadal function in mice with SSHTN. These data demonstrate that high systemic pressure and salt differentially act on end organ immune cells, contributing to the broader understanding of how BP and salt intake collectively shape immune responses and highlight implications for targeted therapeutic interventions., (© 2024 The Author(s).)

Published

2024

35. Utilizing pathophysiological concepts of ischemia-reperfusion injury to design renoprotective strategies and therapeutic interventions for normothermic ex vivo kidney perfusion.

Author

Ogurlu B, Hamelink TL, Van Tricht IM, Leuvenink HGD, De Borst MH, Moers C, and Pool MBF

Subjects

Humans, Kidney blood supply, Kidney physiopathology, Animals, Reperfusion Injury prevention & control, Organ Preservation methods, Kidney Transplantation, Perfusion

Abstract

Normothermic machine perfusion (NMP) has emerged as a promising tool for the preservation, viability assessment, and repair of deceased-donor kidneys prior to transplantation. These kidneys inevitably experience a period of ischemia during donation, which leads to ischemia-reperfusion injury when NMP is subsequently commenced. Ischemia-reperfusion injury has a major impact on the renal vasculature, metabolism, oxygenation, electrolyte balance, and acid-base homeostasis. With an increased understanding of the underlying pathophysiological mechanisms, renoprotective strategies and therapeutic interventions can be devised to minimize additional injury during normothermic reperfusion, ensure the safe implementation of NMP, and improve kidney quality. This review discusses the pathophysiological alterations in the vasculature, metabolism, oxygenation, electrolyte balance, and acid-base homeostasis of deceased-donor kidneys and delineates renoprotective strategies and therapeutic interventions to mitigate renal injury and improve kidney quality during NMP., Competing Interests: Declaration of competing interest The authors of this manuscript have no conflicts of interest to disclose as described by the American Journal of Transplantation., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

36. Virtual Nephron: Evaluation of a Novel Virtual Reality Educational Tool.

Author

Nakhoul GN, Taliercio JJ, Bassil EH, Arrigain S, Schold JD, Wardrop R, O'Toole J, Nally JV, Bierer SB, Sedor JR, and Mehdi A

Abstract

Introduction: Recent technological advancements allowed the development of engaging technological tools. Using ASN funding from the ASN, we developed a 3D Virtual Reality (VR) physiology course entitled DiAL-Neph (Diuretic Action and eLectrolyte transport in the Nephron). We hereby present its evaluation., Methods: The study consisted of 2 parts: evaluation of knowledge gain, and qualitative evaluation of platform reception. Internal medicine PGY1 residents were randomly assigned into 2 groups: a VR group and a conventional group. Knowledge acquisition was assessed with a post-test administered at the end of the course and repeated within 6 to 12 weeks. Independent t-tests were used to compare the number of correct answers between the groups. A survey and focus groups composed of medicine residents evaluated the platform. Sessions were recorded and transcribed verbatim. Data was analyzed through the content analysis approach by two independent reviewers., Results: Of 117 PGY1 resident participants, 64 were randomized to the VR group and 53 were randomized to the traditional group. Initial test results showed higher scores among VR compared to the traditional group (76.5% correct vs. 68.8%). Seventy-eight PGY1s participated in the follow up testing (46 VR group vs. 32 traditional group) and results showed no significant difference in test results. Greater than 90% of the residents rated the platform positively and 77% preferred it as a teaching method., Conclusion: The DiAL-Neph VR platform appeared to improve short-term learning but not long-term retention. Further studies are needed to investigate the impact of such teaching platforms on overall interest in nephrology., (© 2024 International Society of Nephrology. Published by Elsevier Inc.)

Published

2024

37. Editorial: Proteomics, mass spectrometry and bioinformatics in renal pathophysiology.

Author

Cummins, Timothy D. and Thongboonkerd, Visith

Subjects

MASS spectrometry, PROTEOMICS, PATHOLOGICAL physiology, BIOINFORMATICS, DIABETIC nephropathies

Published

2023

38. Collecting Duct Principal Cell Transport Processes and Their Regulation

Author

Pearce, David, Soundararajan, Rama, Trimpert, Christiane, Kashlan, Ossama B, Deen, Peter MT, and Kohan, Donald E

Subjects

Kidney Disease, 1.1 Normal biological development and functioning, Underpinning research, Animals, Aquaporin 2, Body Water, Epithelial Cells, Epithelial Sodium Channels, Humans, Ion Transport, Kidney Tubules, Collecting, Potassium, Potassium Channels, Inwardly Rectifying, Signal Transduction, Sodium, Sodium-Potassium-Exchanging ATPase, Water-Electrolyte Balance, renal physiology, collecting duct, principal cell, epithelial cell, Clinical Sciences, Urology & Nephrology

Abstract

The principal cell of the kidney collecting duct is one of the most highly regulated epithelial cell types in vertebrates. The effects of hormonal, autocrine, and paracrine factors to regulate principal cell transport processes are central to the maintenance of fluid and electrolyte balance in the face of wide variations in food and water intake. In marked contrast with the epithelial cells lining the proximal tubule, the collecting duct is electrically tight, and ion and osmotic gradients can be very high. The central role of principal cells in salt and water transport is reflected by their defining transporters-the epithelial Na(+) channel (ENaC), the renal outer medullary K(+) channel, and the aquaporin 2 (AQP2) water channel. The coordinated regulation of ENaC by aldosterone, and AQP2 by arginine vasopressin (AVP) in principal cells is essential for the control of plasma Na(+) and K(+) concentrations, extracellular fluid volume, and BP. In addition to these essential hormones, additional neuronal, physical, and chemical factors influence Na(+), K(+), and water homeostasis. Notably, a variety of secreted paracrine and autocrine agents such as bradykinin, ATP, endothelin, nitric oxide, and prostaglandin E2 counterbalance and limit the natriferic effects of aldosterone and the water-retaining effects of AVP. Considerable recent progress has improved our understanding of the transporters, receptors, second messengers, and signaling events that mediate principal cell responses to changing environments in health and disease. This review primarily addresses the structure and function of the key transporters and the complex interplay of regulatory factors that modulate principal cell ion and water transport.

Published

2015

39. Salt‐Sensitive Hypertension, Renal Injury, and Renal Vasodysfunction Associated With Dahl Salt‐Sensitive Rats Are Abolished in Consomic SS.BN1 Rats

Author

Jacqueline C. Potter, Shannon A. Whiles, Conor B. Miles, Jenna B. Whiles, Mark A. Mitchell, Brianna E. Biederman, Febronia M. Dawoud, Kevin F. Breuel, Geoffrey A. Williamson, Maria M. Picken, and Aaron J. Polichnowski

Subjects

blood flow regulation, blood pressure, kidney, renal physiology, salt‐sensitivity hypertension, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Background Abnormal renal hemodynamic responses to salt‐loading are thought to contribute to salt‐sensitive (SS) hypertension. However, this is based largely on studies in anesthetized animals, and little data are available in conscious SS and salt‐resistant rats. Methods and Results We assessed arterial blood pressure, renal function, and renal blood flow during administration of a 0.4% NaCl and a high‐salt (4.0% NaCl) diet in conscious, chronically instrumented 10‐ to 14‐week‐old Dahl SS and consomic SS rats in which chromosome 1 from the salt‐resistant Brown‐Norway strain was introgressed into the genome of the SS strain (SS.BN1). Three weeks of high salt intake significantly increased blood pressure (20%) and exacerbated renal injury in SS rats. In contrast, the increase in blood pressure (5%) was similarly attenuated in Brown‐Norway and SS.BN1 rats, and both strains were completely protected against renal injury. In SS.BN1 rats, 1 week of high salt intake was associated with a significant decrease in renal vascular resistance (−8%) and increase in renal blood flow (15%). In contrast, renal vascular resistance failed to decrease, and renal blood flow remained unchanged in SS rats during high salt intake. Finally, urinary sodium excretion and glomerular filtration rate were similar between SS and SS.BN1 rats during 0.4% NaCl and high salt intake. Conclusions Our data support the concept that renal vasodysfunction contributes to blood pressure salt sensitivity in Dahl SS rats, and that genes on rat chromosome 1 play a major role in modulating renal hemodynamic responses to salt loading and salt‐induced hypertension.

Published

2021

40. Renal Physiology

Author

Khatib, Reem, Farag, Ehab, editor, Argalious, Maged, editor, Tetzlaff, John E., editor, and Sharma, Deepak, editor

Published

2018

41. Studies from Icahn School of Medicine at Mount Sinai Update Current Data on Health and Medicine (GDF15, an Emerging Player in Renal Physiology and Pathophysiology).

Abstract

A recent report from the Icahn School of Medicine at Mount Sinai discusses the emerging role of the growth factor GDF15 in renal physiology and pathophysiology. GDF15 has been found to play a role in various biological processes and is now considered a stress-related hormone. The research highlights the involvement of GDF15 in kidney functions and its association with chronic kidney disease, diabetic nephropathy, and renal cancer. The report also explores the role of GDF15 in maintaining renal homeostasis. For more information, the full article can be accessed through the International Journal of Molecular Sciences. [Extracted from the article]

Published

2024

42. From Proteinuria to Fibrosis: An Update on Pathophysiology and Treatment Options.

Author

Sharma, Sonia and Smyth, Brendan

Subjects

*PROTEINURIA, *KIDNEY failure, *RENAL fibrosis, *CONGENITAL disorders, *CHRONIC kidney failure, *KIDNEY tubules, *KIDNEY diseases

Abstract

Background: Proteinuria is a key biomarker in nephrology. It is central to diagnosis and risk assessment and the primary target of many important therapies. Etiologies resulting in pathological proteinuria include congenital and acquired disorders, as well as both glomerular (immune/non-immune mediated) and tubular defects. Summary: Untreated proteinuria is strongly linked to progressive loss of kidney function and kidney failure. Excess protein reaching the renal tubules is ordinarily resorbed by the tubular epithelium. However, when these mechanisms are overwhelmed, a variety of inflammatory and fibrotic pathways are activated, causing both interstitial fibrosis and glomerulosclerosis. Nevertheless, the specific mechanisms underlying this are complex and remain incompletely understood. Recently, a number of treatments, in addition to angiotensin system blockade, have been shown to effectively slow the progression of proteinuric chronic kidney disease. However, additional therapies are clearly needed. Key message: This review provides an update on the pathophysiology of proteinuria, the pathways leading to fibrosis, and an overview of current and emerging therapies. [ABSTRACT FROM AUTHOR]

Published

2021

43. Kidney physiology and pathophysiology during heat stress and the modification by exercise, dehydration, heat acclimation and aging.

Author

Chapman, Christopher L., Johnson, Blair D., Parker, Mark D., Hostler, David, Pryor, Riana R., and Schlader, Zachary

Subjects

*KIDNEY physiology, *PHYSIOLOGICAL effects of heat, *FEVER, *KIDNEY function tests, *ACUTE kidney failure, *DEHYDRATION, *OLDER people

Abstract

The kidneys' integrative responses to heat stress aid thermoregulation, cardiovascular control, and water and electrolyte regulation. Recent evidence suggests the kidneys are at increased risk of pathological events during heat stress, namely acute kidney injury (AKI), and that this risk is compounded by dehydration and exercise. This heat stress related AKI is believed to contribute to the epidemic of chronic kidney disease (CKD) occurring in occupational settings. It is estimated that AKI and CKD affect upwards of 45 million individuals in the global workforce. Water and electrolyte disturbances and AKI, both of which are representative of kidney-related pathology, are the two leading causes of hospitalizations during heat waves in older adults. Structural and physiological alterations in aging kidneys likely contribute to this increased risk. With this background, this comprehensive narrative review will provide the first aggregation of research into the integrative physiological response of the kidneys to heat stress. While the focus of this review is on the human kidneys, we will utilize both human and animal data to describe these responses to passive and exercise heat stress, and how they are altered with heat acclimation. Additionally, we will discuss recent studies that indicate an increased risk of AKI due to exercise in the heat. Lastly, we will introduce the emerging public health crisis of older adults during extreme heat events and how the aging kidneys may be more susceptible to injury during heat stress. [ABSTRACT FROM AUTHOR]

Published

2021

44. To pee and to poo: Cross-organ principles and mechanisms in renal and gastrointestinal physiology

Author

Hwee-Ming Cheng and See-Ziau Hoe

Subjects

Cross-organ principles, gastrointestinal physiology, integration, renal physiology, Therapeutics. Pharmacology, RM1-950

Abstract

Cross-organ principles can be recognized and taught as an expression of the shared functional symmetry and common design in physiology. This integrated concept will help students to appreciate the unifying mechanisms that maintain the homeostatic balance in the body. In this article, the cross-organ similarities in gastrointestinal and renal physiology are extracted to aid learning and teaching. Some fun conversations between the Kiddo Urinary (U) and the Gastro Intestinal (I) are included to promote enjoyment in physiology.

Published

2019

45. WNKs are potassium-sensitive kinases.

Author

Pleinis, John M., Norrell, Logan, Akella, Radha, Humphreys, John M., Haixia He, Qifei Sun, Feng Zhang, Sosa-Pagan, Jason, Morrison, Daryl E., Schellinger, Jeffrey N., Jackson, Laurie K., Goldsmith, Elizabeth J., and Rodan, Aylin R.

Subjects

*POTASSIUM ions, *KINASES, *HIGH-potassium diet, *CHLORIDE channels, *CHLORIDE ions, *BLOOD pressure

Abstract

With no lysine (K) (WNK) kinases regulate epithelial ion transport in the kidney to maintain homeostasis of electrolyte concentrations and blood pressure. Chloride ion directly binds WNK kinases to inhibit autophosphorylation and activation. Changes in extracellular potassium are thought to regulate WNKs through changes in intracellular chloride. Prior studies demonstrate that in some distal nephron epithelial cells, intracellular potassium changes with chronic low- or high-potassium diet. We, therefore, investigated whether potassium regulates WNK activity independent of chloride. We found decreased activity of Drosophila WNK and mammalian WNK3 and WNK4 in fly Malpighian (renal) tubules bathed in high extracellular potassium, even when intracellular chloride was kept constant at either -13mM or 26 mM. High extracellular potassium also inhibited chloride-insensitive mutants of WNK3 and WNK4. High extracellular rubidium was also inhibitory and increased tubule rubidium. The Naþ/Kþ- ATPase inhibitor, ouabain, which is expected to lower intracellular potassium, increased tubule Drosophila WNK activity. In vitro, potassium increased the melting temperature of Drosophila WNK, WNK1, and WNK3 kinase domains, indicating ion binding to the kinase. Potassium inhibited in vitro autophosphorylation of Drosophila WNK and WNK3, and also inhibited WNK3 and WNK4 phosphorylation of their substrate, Ste20-related proline/alanine-rich kinase (SPAK). The greatest sensitivity of WNK4 to potassium occurred in the range of 80-180 mM, encompassing physiological intracellular potassium concentrations. Together, these data indicate chloride-independent potassium inhibition of Drosophila and mammalian WNK kinases through direct effects of potassium ion on the kinase. [ABSTRACT FROM AUTHOR]

Published

2021

46. Lysophosphatidic acid (LPA) as a modulator of plasma membrane Ca2+-ATPase from basolateral membranes of kidney proximal tubules.

Author

Sant'Anna, Julliana F., Baldez, Vanessa S., Razuck-Garrão, Natalie A., Lemos, Thiago, Diaz, Bruno L., and Einicker-Lamas, Marcelo

Abstract

Lysophosphatidic acid (LPA) acts through the activation of G protein-coupled receptors, in a Ca2+-dependent manner. We show the effects of LPA on the plasma membrane Ca2+-ATPase (PMCA) from kidney proximal tubule cells. The Ca2+-ATPase activity was inhibited by nanomolar concentrations of LPA, with maximal inhibition (~50%) obtained with 20 nM LPA. This inhibitory action on PMCA activity was blocked by Ki16425, an antagonist for LPA receptors, indicating that this lipid acts via LPA1 and/or LPA3 receptor. This effect is PKC-dependent, since it is abolished by calphostin C and U73122, PKC, and PLC inhibitors, respectively. Furthermore, the addition of 10−8 M PMA, a well-known PKC activator, mimicked PMCA modulation by LPA. We also demonstrated that the PKC activation leads to an increase in PMCA phosphorylation. These results indicate that LPA triggers LPA1 and/or LPA3 receptors at the BLM, inducing PKC-dependent phosphorylation with further inhibition of PMCA. Thus, LPA is part of the regulatory lipid network present at the BLM and plays an important role in the regulation of intracellular Ca2+ concentration that may result in significant physiological alterations in other Ca2+-dependent events ascribed to the renal tissue. [ABSTRACT FROM AUTHOR]

Published

2021

47. Molecular characteristics and physiological roles of Na+–K+–Cl− cotransporter 2.

Author

Marcoux, Andree‐Anne, Tremblay, Laurence E., Slimani, Samira, Fiola, Marie‐Jeanne, Mac‐Way, Fabrice, Garneau, Alexandre P., and Isenring, Paul

Subjects

*ION transport (Biology), *MEMBRANE proteins, *KIDNEY tubules, *HYPERTENSION

Abstract

Na+–K+–Cl− cotransporter 2 (NKCC2; SLC12A1) is an integral membrane protein that comes as three splice variants and mediates the cotranslocation of Na+, K+, and Cl− ions through the apical membrane of the thick ascending loop of Henle (TALH). In doing so, and through the involvement of other ion transport systems, it allows this nephron segment to reclaim a large fraction of the ultrafiltered Na+, Cl−, Ca2+, Mg2+, and HCO3− loads. The functional relevance of NKCC2 in human is illustrated by the many abnormalities that result from the inactivation of this transport system through the use of loop diuretics or in the setting of inherited disorders. The following presentation aims at discussing the physiological roles and molecular characteristics of Na+–K+–Cl− cotransport in the TALH and those of the individual NKCC2 splice variants more specifically. Many of the historical and recent data that have emerged from the experiments conducted will be outlined and their larger meaning will also be placed into perspective with the aid of various hypotheses. [ABSTRACT FROM AUTHOR]

Published

2021

48. Intravital Imaging with Two-Photon Microscopy: A Look into the Kidney

Author

Vincenzo Costanzo and Michele Costanzo

Subjects

intravital imaging, two-photon microscopy, kidney disease, renal physiology, machine learning, Applied optics. Photonics, TA1501-1820

Abstract

Fluorescence microscopy has represented a crucial technique to explore the cellular and molecular mechanisms in the field of biomedicine. However, the conventional one-photon microscopy exhibits many limitations when living samples are imaged. The new technologies, including two-photon microscopy (2PM), have considerably improved the in vivo study of pathophysiological processes, allowing the investigators to overcome the limits displayed by previous techniques. 2PM enables the real-time intravital imaging of the biological functions in different organs at cellular and subcellular resolution thanks to its improved laser penetration and less phototoxicity. The development of more sensitive detectors and long-wavelength fluorescent dyes as well as the implementation of semi-automatic software for data analysis allowed to gain insights in essential physiological functions, expanding the frontiers of cellular and molecular imaging. The future applications of 2PM are promising to push the intravital microscopy beyond the existing limits. In this review, we provide an overview of the current state-of-the-art methods of intravital microscopy, focusing on the most recent applications of 2PM in kidney physiology.

Published

2022

49. A meme-based approach for enhancing student engagement and learning in renal physiology.

Author

Subbiramaniyan, Vivekananth, Apte, Chandrashekhar, and Mohammed, Ciraj Ali

Subjects

*KIDNEY physiology, *STUDENT engagement, *LEARNING Management System, *COLLEGE curriculum, *SOCIAL interaction

Abstract

As educators around the world are exploring new approaches to keep students involved in remote learning during the pandemic, we investigated the utility of memes in promoting engagement in the online environment. Medical students enrolled in a human physiology course at the College of Medicine and Health Sciences, Sohar, Oman were provided with an option to create memes related to the learning outcomes in renal physiology. One hundred forty-six of 280 students chose to create memes (52%), and the remaining students chose to submit either a labeled diagram or a concept map. Students uploaded their work in the discussion forum of the learning management system. All students enrolled in the course were given an opportunity for interaction with the uploaded content by commenting and upvoting thereafter. Students were requested to give anonymous feedback on their experience specifically on the activity related to memes. Feedback received from 142 of 280 students through anonymous comments was subjected to thematic analysis. Based on the analysis of the data, we found that memes elicited interest in the topic, facilitated peer interaction, simplified complex ideas, enhanced retention of associated concepts, and fostered a positive learning environment. [ABSTRACT FROM AUTHOR]

Published

2022

50. Novel Fanconi renotubular syndromes provide insights in proximal tubule pathophysiology.

Author

Lemaire, Mathieu

Abstract

The various forms of Fanconi renotubular syndromes (FRTS) offer significant challenges for clinicians and present unique opportunities for scientists who study proximal tubule physiology. This review will describe the clinical characteristics, genetic underpinnings, and underlying pathophysiology of the major forms of FRST. Although the classic forms of FRTS will be presented (e.g., Dent disease or Lowe syndrome), particular attention will be paid to five of the most recently discovered FRTS subtypes caused by mutations in the genes encoding for L-arginine:glycine amidinotransferase (GATM), solute carrier family 34 (type Ii sodium/phosphate cotransporter), member 1 (SLC34A1), enoyl-CoAhydratase/3-hydroxyacyl CoA dehydrogenase (EHHADH), hepatocyte nuclear factor 4A (HNF4A), or NADH dehydrogenase complex I, assembly factor 6 (NDUFAF6). We will explore how mutations in these genes revealed unexpected mechanisms that led to compromised proximal tubule functions. We will also describe the inherent challenges associated with gene discovery studies based on findings derived from small, single-family studies by focusing the story of FRTS type 2 (SLC34A1). Finally, we will explain how extensive alternative splicing of HNF4A has resulted in confusion with mutation nomenclature for FRTS type 4. [ABSTRACT FROM AUTHOR]

Published

2021