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497,551 results on '"Kidney"'

68. The association between bone density of lumbar spines and different daily protein intake in different renal function.

Author

Lee, Chia-Lin, Chen, Kun-Hui, Liu, Wei-Ju, Chen, Ching-Hsien, and Tsai, Shang-Feng

Subjects
Bone density, chronic kidney disease, lumbar spine, osteoporosis, protein diet, Humans, Bone Density, Nutrition Surveys, Osteoporosis, Kidney, Renal Insufficiency, Chronic, Dietary Proteins
Abstract

BACKGROUND: Low protein intake (LPI) has been suggested as a treatment for chronic kidney disease (CKD). However, protein intake is essential for bone health. METHODS: We studied the database of the National Health and Nutrition Examination Survey, 2005-2010. Basic variables, metabolic diseases, and bone density of different femoral areas were stratified into four subgroups according to different protein intake (DPI) (that is, 1.2 g/kg/day). RESULTS: Significant differences were found among all lumbar area bone mineral density (BMD) and T-scores (p 1.2 g/day/kg over L2 (relative risk (RR)=1.326, 95% confidence interval (CI)=1.062-1.656), subgroup >1.2 g/day/kg over L3 (RR = 1.31, 95%CI = 1.057-1.622), subgroup 1.2 g/day/kg over all L spines (RR = 0.333, 95%CI = 1.098-1.618). However, a higher risk of osteoporosis was observed only in the non-CKD group. There was an apparent trend of higher DPI coexisting with lower BMD and T scores in patients with CKD. For osteoporosis (reference:0.8-1.0 g/day/kg), lower (1.2 g/day/kg) was associated with higher risks in the non-CKD group, but not in the CKD group. CONCLUSIONS: In the CKD group, LPI for renal protection was safe without threatening L spine bone density and without causing a higher risk of osteoporosis.

Published
2024

70. Epidemiology of sepsis-associated acute kidney injury in critically ill patients: a multicenter, prospective, observational cohort study in South Korea.

Author

Song, Myung, Jang, Yeonhoon, Legrand, Matthieu, Park, Sunghoon, Ko, RyoungEun, Suh, Gee, Oh, Dong, Lee, Su, Park, Mi, Lim, Chae-Man, Jung, Se, and Lim, Sung

Subjects
Acute kidney injury, Epidemiology, Intensive care unit, Kidney, Sepsis, Humans, Prospective Studies, Male, Republic of Korea, Sepsis, Female, Acute Kidney Injury, Middle Aged, Aged, Critical Illness, Intensive Care Units, Cohort Studies, Hospital Mortality, Risk Factors, Incidence, Adult
Abstract

BACKGROUND: Despite the clinical importance of sepsis-associated acute kidney injury (SA-AKI), little is known about its epidemiology. We aimed to investigate the incidence and outcomes of SA-AKI, as well as the risk factors for mortality among patients with severe SA-AKI in critically ill patients. METHODS: This secondary multicenter, observational, prospective cohort analysis of sepsis in South Korea evaluated patients aged ≥ 19 years admitted to intensive care units with a diagnosis of sepsis. The primary outcome was the incidence of SA-AKI, defined using the new consensus definition of the Acute Disease Quality Initiative 28 Workgroup. Secondary outcomes were in-hospital mortality and risk factors for in-hospital mortality. RESULTS: Between September 2019 and December 2022, 5100 patients were admitted to intensive care units with a diagnosis of sepsis, and 3177 (62.3%) developed SA-AKI. A total of 613 (19.3%), 721 (22.7%), and 1843 (58.0%) patients had stage 1, 2, and 3 SA-AKI, respectively. Severe SA-AKI (stages 2 and 3 combined) was associated with an increased risk of in-hospital mortality. Adherence to the fluid resuscitation component of the one-hour sepsis bundle was associated with a decreased risk of in-hospital mortality in severe SA-AKI (adjusted odds ratio, 0.62; 95% confidence interval, 0.48-0.79; P

Published
2024

71. The urine protein/creatinine ratio as a reliable indicator of 24-h urine protein excretion across different levels of renal function and proteinuria: the TUNARI prospective study.

Author

Gutiérrez-Peredo, Gabriel, Montaño-Castellón, Iris, Gutiérrez-Peredo, Andrea, Lopes, Marcelo, Tapioca, Fernanda, Guimaraes, Maria, Montaño-Castellón, Sony, Guedes, Sammara, da Costa, Fernanda, Mattoso, Ricardo, Filho, José, Norris, Keith, de Almeida, Antonio, and Lopes, Antonio

Subjects
24-h urine protein, Nephrology, Proteinuria creatinine ratio, Renal function, Humans, Proteinuria, Female, Male, Cross-Sectional Studies, Creatinine, Adult, Middle Aged, Prospective Studies, Sensitivity and Specificity, ROC Curve, Kidney, Glomerular Filtration Rate
Abstract

BACKGROUND: The 24-h urine protein (24-hUP) excretion is the gold standard for evaluating proteinuria. This study aimed to evaluate the diagnostic efficacy of protein/creatinine ratio (PCR) for estimating 24-hUP at various levels of renal function and proteinuria levels. METHODS: A cross-sectional study was conducted between December 2021 and December 2023 in Salvador, Bahia-Brazil, as an extension of previously published data from the TUNARI study. The study included 217 samples from 152 patients with various levels of renal function and proteinuria. PCR in isolated samples and 24-hUP were determined conventionally within a 24-h timeframe. Patients were classified into three groups according to the level of renal function (Group 1 = 10 to  60 mL/min) and level of proteinuria ( 3.5 g/day). The data were analyzed using the Spearman correlation (rs), coefficient of determination (r2), Bland-Altman plots and receiver operating characteristic (ROC) curve. Likelihood ratios, positive (LR +), and negative (LR-) were derived from the sensitivity and specificity of PCR. RESULTS: Mean age was 41.5 ± 15.7 years, 61.8% were women, 36.8% Black and 52% Mixed-race. Glomerulopathies constituted 80.3%; 46.1% with lupus nephritis. Of the total urine samples, we observed a high correlation between PCR in the total sample of 24-hUP sample (rs = 0.86, p  0.3-3.5 g/day, the sensitivity was 64.1%, the specificity was 84.6%, and the AUC was 0.76 (95% CI = 0.67; 0.84), PCR detected all cases > 3.5 g/day. CONCLUSIONS: PCR is a suitable measure to be used as an indicator of 24-hUP at different levels of renal function, but may have limitations at higher levels of proteinuria. Analysis of PCR by proteinuria level found that agreement as well as sensitivity decreases at higher levels, but it maintains good specificity and is able to identify nephrotic range proteinuria.

Published
2024

72. The RSNA Abdominal Traumatic Injury CT (RATIC) Dataset.

Author

Rudie, Jeffrey, Lin, Hui-Ming, Ball, Robyn, Jalal, Sabeena, Prevedello, Luciano, Nicolaou, Savvas, Marinelli, Brett, Flanders, Adam, Magudia, Kirti, Shih, George, Davis, Melissa, Mongan, John, Chang, Peter, Berger, Ferco, Hermans, Sebastiaan, Law, Meng, Richards, Tyler, Grunz, Jan-Peter, Kunz, Andreas, Mathur, Shobhit, Galea-Soler, Sandro, Chung, Andrew, Afat, Saif, Kuo, Chin-Chi, Aweidah, Layal, Villanueva Campos, Ana, Somasundaram, Arjuna, Sanchez Tijmes, Felipe, Jantarangkoon, Attaporn, Kayat Bittencourt, Leonardo, Brassil, Michael, El Hajjami, Ayoub, Dogan, Hakan, Becircic, Muris, Bharatkumar, Agrahara, Júdice de Mattos Farina, Eduardo, and Colak, Errol

Subjects
CT, Kidney, Large Bowel, Liver, Small Bowel, Spleen, Trauma, Humans, Abdominal Injuries, Tomography, X-Ray Computed, Male, Female, Adult
Abstract

Supplemental material is available for this article.

Published
2024

73. Absence of Kidney Tubular Injury in Patients With Acute Heart Failure With Acute Kidney Injury.

Author

Duff, Stephen, Wettersten, Nicholas, Horiuchi, Yu, van Veldhuisen, Dirk, Raturi, Sagar, Irwin, Ruairi, Côté, Jean, Maisel, Alan, Ix, Joachim, and Murray, Patrick

Subjects
acute kidney injury, blood pressure, epidermal growth factor, galectin 3, kidney, Humans, Male, Female, Heart Failure, Biomarkers, Aged, Acute Kidney Injury, Middle Aged, Kidney Tubules, Galectin 3, Acute Disease, Epidermal Growth Factor, Aged, 80 and over, Risk Factors, Blood Proteins, Galectins
Abstract

BACKGROUND: Worsening renal function (WRF) is common in hospitalized patients being treated for acute heart failure. However, discriminating clinically significant WRF remains challenging. In patients hospitalized with acute heart failure, we evaluated if blood and urine biomarkers of cardiac and kidney dysfunction were associated with adverse outcomes. METHODS: We identified 175 of 927 participants in the AKINESIS study (Acute Kidney Neutrophil Gelatinase-Associated Lipocalin Evaluation of Symptomatic Heart Failure Study) who met criteria for stage 1 or 2 Kidney Disease: Improvement Global Outcomes acute kidney injury during the first 3 days of hospitalization. We measured 24 blood and urine biomarkers from specimens collected within 24 hours of meeting acute kidney injury criteria. The primary composite outcome consisted of worsening WRF (higher acute kidney injury stage), need for dialysis, or death at 30 days. Biomarkers association with the composite outcome was assessed with logistic regression by tertiles and area under the curve (AUC). RESULTS: Of the 175 participants, 32 (18%) developed the primary composite outcome. Only history of chronic kidney disease was significantly different between those with and without the composite outcome. The highest tertile of plasma Gal-3 (galectin-3) and urine epidermal growth factor were associated with increased odds of the composite outcome compared with the lowest tertile in unadjusted analyses. After adjusting for serum creatinine, systolic blood pressure, and blood urea nitrogen, only the highest tertile of Gal-3 was associated with greater odds of the composite outcome (odds ratio, 4.6 [95% CI, 1.4-16.0). Gal-3 had the highest AUC (0.70 [95% CI, 0.58-0.82]), while epidermal growth factor had a lower AUC (0.63 [95% CI, 0.53-0.74]). Notably, urine biomarkers of kidney tubule injury were not associated with the composite outcome. CONCLUSIONS: Tubular injury does not occur in most patients with acute heart failure experiencing WRF, consistent with the functional mechanisms of WRF in this patient population. REGISTRATION: URL: https://www.clinicaltrials.gov/study/NCT01291836?term=NCT01291836&rank=1; Unique identifier: NCT01291836.

Published
2024

74. Paraneoplastic renal dysfunction in fly cancer models driven by inflammatory activation of stem cells

Author

Kwok, Sze Hang, Liu, Yuejiang, Bilder, David, and Kim, Jung

Subjects
Biomedical and Clinical Sciences, Immunology, Kidney Disease, Cancer, 2.1 Biological and endogenous factors, Renal and urogenital, Animals, Stem Cells, Disease Models, Animal, Inflammation, Humans, Kidney Tubules, Drosophila melanogaster, Kidney Diseases, Kidney, Paraneoplastic Syndromes, Animals, Genetically Modified, Interleukin-6, Drosophila, cancer model, kidney, paraneoplasia, tumor–host
Abstract

Tumors can induce systemic disturbances in distant organs, leading to physiological changes that enhance host morbidity. In Drosophila cancer models, tumors have been known for decades to cause hypervolemic "bloating" of the abdominal cavity. Here we use allograft and transgenic tumors to show that hosts display fluid retention associated with autonomously defective secretory capacity of fly renal tubules, which function analogous to those of the human kidney. Excretion from these organs is blocked by abnormal cells that originate from inappropriate activation of normally quiescent renal stem cells (RSCs). Blockage is initiated by IL-6-like oncokines that perturb renal water-transporting cells and trigger a damage response in RSCs that proceeds pathologically. Thus, a chronic inflammatory state produced by the tumor causes paraneoplastic fluid dysregulation by altering cellular homeostasis of host renal units.

Published
2024

75. Sulfotransferase 1C2 Increases Mitochondrial Respiration by Converting Mitochondrial Membrane Cholesterol to Cholesterol Sulfate.

Author

Kolb, Alexander, Corridon, Peter, Ullah, Mahbub, Pfaffenberger, Zechariah, Xu, Wei, Winfree, Seth, Sandoval, Ruben, Hato, Takeshi, Witzmann, Frank, Mohallem, Rodrigo, Franco, Jackeline, Aryal, Uma, Atkinson, Simon, Basile, David, and Bacallao, Robert

Subjects
Animals, Cholesterol, Sulfotransferases, Mitochondria, Cholesterol Esters, Mitochondrial Membranes, Mice, Cell Respiration, Male, Membrane Potential, Mitochondrial, Kidney, Mice, Inbred C57BL
Abstract

HYPOTHESIS: In this communication, we test the hypothesis that sulfotransferase 1C2 (SULT1C2, UniProt accession no. Q9WUW8) can modulate mitochondrial respiration by increasing state-III respiration. METHODS AND RESULTS: Using freshly isolated mitochondria, the addition of SULT1C2 and 3-phosphoadenosine 5 phosphosulfate (PAPS) results in an increased maximal respiratory capacity in response to the addition of succinate, ADP, and rotenone. Lipidomics and thin-layer chromatography of mitochondria treated with SULT1C2 and PAPS showed an increase in the level of cholesterol sulfate. Notably, adding cholesterol sulfate at nanomolar concentration to freshly isolated mitochondria also increases maximal respiratory capacity. In vivo studies utilizing gene delivery of SULT1C2 expression plasmids to kidneys result in increased mitochondrial membrane potential and confer resistance to ischemia/reperfusion injury. Mitochondria isolated from gene-transduced kidneys have elevated state-III respiration as compared with controls, thereby recapitulating results obtained with mitochondrial fractions treated with SULT1C2 and PAPS. CONCLUSION: SULT1C2 increases mitochondrial respiratory capacity by modifying cholesterol, resulting in increased membrane potential and maximal respiratory capacity. This finding uncovers a unique role of SULT1C2 in cellular physiology and extends the role of sulfotransferases in modulating cellular metabolism.

Published
2024

76. Elevation of Donor-derived Cell-free DNA Before Biopsy-proven Rejection in Kidney Transplant.

Author

Bromberg, Jonathan, Bunnapradist, Suphamai, Samaniego-Picota, Milagros, Anand, Sanjiv, Stites, Erik, Gauthier, Philippe, Demko, Zachary, Prewett, Adam, Armer-Cabral, Madeleine, Marshall, Kyle, Kaur, Navchetan, Bloom, Michelle, Tabriziani, Hossein, Bhorade, Sangeeta, and Cooper, Matthew

Subjects
Humans, Kidney Transplantation, Graft Rejection, Cell-Free Nucleic Acids, Male, Female, Middle Aged, Retrospective Studies, Biopsy, Biomarkers, Adult, Tissue Donors, Kidney, Registries, Creatinine, Aged, Time Factors, Predictive Value of Tests, Prospective Studies
Abstract

BACKGROUND: Standard-of-care biomarkers for renal allograft rejection are lagging indicators, signaling existing organ injury. This precludes early intervention, when immunological cascades leading to rejection are most susceptible. Donor-derived cell-free DNA (dd-cfDNA) shows promise as an early indicator of rejection, allowing earlier and possibly more effective treatment. This analysis was designed to assess this promise using real-world dd-cfDNA testing evidence. METHODS: This retrospective analysis of the prospective, observational ProActive registry study (NCT04091984) assessed dd-cfDNA and serum creatinine levels before biopsy in 424 patients with ≥1 dd-cfDNA test (n = 1013) in the 6 mo before biopsy. RESULTS: Of 4667 enrolled patients, 1631 patients had ≥18 mo of follow-up data, of which 424 had a biopsy and were included in this analysis. Twenty-six biopsies showed antibody-mediated rejection (ABMR), 62 showed T cell-mediated rejection, and 336 showed nonrejection; each from a unique patient. dd-cfDNA fractions were significantly elevated 5 mo before ABMR biopsies, and 2 mo before T cell-mediated rejection biopsies, compared with nonrejection biopsies. In contrast, serum creatinine did not discriminate between rejection and nonrejection in advance, or concurrent with biopsy. Among patients with nonrejection biopsies, estimated glomerular filtration rate was significantly lower in cases with ≥2 increased dd-cfDNA results (≥1%), compared with those with 0 or 1 increased dd-cfDNA result. CONCLUSIONS: These data indicate that dd-cfDNA is an early indicator of biopsy-proven rejection, especially ABMR, suggesting a greater role for dd-cfDNA in surveillance to identify patients at high risk of ongoing or future rejection, thus requiring closer monitoring, biopsy, or other management changes.

Published
2024

77. PTER is a N-acetyltaurine hydrolase that regulates feeding and obesity.

Author

Wei, Wei, Lyu, Xuchao, Markhard, Andrew, Fu, Sipei, Mardjuki, Rachel, Cavanagh, Peter, Zeng, Xianfeng, Rajniak, Jakub, Lu, Nannan, Xiao, Shuke, Zhao, Meng, Moya-Garzon, Maria, Truong, Steven, Chou, Jonathan, Wat, Lianna, Chidambaranathan-Reghupaty, Saranya, Coassolo, Laetitia, Xu, Duo, Shen, Fangfang, Huang, Wentao, Ramirez, Cuauhtemoc, Jang, Cholsoon, Li, Lingyin, Svensson, Katrin, Fischbach, Michael, and Long, Jonathan

Subjects
Animals, Female, Humans, Male, Mice, Eating, Glucose, Homeostasis, Hydrolases, Hydrolysis, Kidney, Liver, Mice, Inbred C57BL, Mice, Knockout, Obesity, Taurine, Carrier Proteins, Acetic Acid, Exercise, Body Mass Index, Weight Loss, Secondary Metabolism, Energy Metabolism, Body Weight, Brain Stem
Abstract

Taurine is a conditionally essential micronutrient and one of the most abundant amino acids in humans1-3. In endogenous taurine metabolism, dedicated enzymes are involved in the biosynthesis of taurine from cysteine and in the downstream metabolism of secondary taurine metabolites4,5. One taurine metabolite is N-acetyltaurine6. Levels of N-acetyltaurine are dynamically regulated by stimuli that alter taurine or acetate flux, including endurance exercise7, dietary taurine supplementation8 and alcohol consumption6,9. So far, the identities of the enzymes involved in N-acetyltaurine metabolism, and the potential functions of N-acetyltaurine itself, have remained unknown. Here we show that the body mass index associated orphan enzyme phosphotriesterase-related (PTER)10 is a physiological N-acetyltaurine hydrolase. In vitro, PTER catalyses the hydrolysis of N-acetyltaurine to taurine and acetate. In mice, PTER is expressed in the kidney, liver and brainstem. Genetic ablation of Pter in mice results in complete loss of tissue N-acetyltaurine hydrolysis activity and a systemic increase in N-acetyltaurine levels. After stimuli that increase taurine levels, Pter knockout mice exhibit reduced food intake, resistance to diet-induced obesity and improved glucose homeostasis. Administration of N-acetyltaurine to obese wild-type mice also reduces food intake and body weight in a GFRAL-dependent manner. These data place PTER into a central enzymatic node of secondary taurine metabolism and uncover a role for PTER and N-acetyltaurine in body weight control and energy balance.

Published
2024

78. Ensembled SegNeXt Based Glomeruli Segmentation

Author

Kumar, Amit, Das, Dev Kumar, Deotale, Gunjan, Dalimkar, Vedant, Thomas, Tijo, Singhal, Nitin, Goos, Gerhard, Series Editor, Hartmanis, Juris, Founding Editor, Bertino, Elisa, Editorial Board Member, Gao, Wen, Editorial Board Member, Steffen, Bernhard, Editorial Board Member, Yung, Moti, Editorial Board Member, Huo, Yuankai, editor, Millis, Bryan A., editor, Zhou, Yuyin, editor, Younis, Khaled, editor, Wang, Xiao, editor, and Tang, Yucheng, editor

Published
2025
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79. Similar rate of venous thromboembolism (VTE) and failure of non-operative management for early versus delayed VTE chemoprophylaxis in adolescent blunt solid organ injuries: a propensity-matched analysis.

Author

Grigorian, Areg, Schubl, Sebastian, Swentek, Lourdes, Barrios, Cristobal, Lekawa, Michael, Russell, Dylan, and Nahmias, Jeffry

Subjects
Blunt solid organ injury, Deep vein thrombosis, Pediatric trauma, Pulmonary embolism, Venous thromboembolism chemoprophylaxis, Humans, Adolescent, Venous Thromboembolism, Wounds, Nonpenetrating, Female, Male, Propensity Score, Child, Anticoagulants, Retrospective Studies, Spleen, Injury Severity Score, Chemoprevention, Liver, Kidney
Abstract

BACKGROUND: Early initiation of venous thromboembolism (VTE) chemoprophylaxis in adults with blunt solid organ injury (BSOI) has been demonstrated to be safe but this is controversial in adolescents. We hypothesized that adolescent patients with BSOI undergoing non-operative management (NOM) and receiving early VTE chemoprophylaxis (eVTEP) (≤ 48 h) have a decreased rate of VTE and similar rate of failure of NOM, compared to similarly matched adolescents receiving delayed VTE chemoprophylaxis (dVTEP) (> 48 h). METHODS: The 2017-2019 Trauma Quality Improvement Program database was queried for adolescents (12-17 years of age) with BSOI (liver, kidney, and/or spleen) undergoing NOM. We compared eVTEP versus dVTEP using a 1:1 propensity score model, matching for age, comorbidities, BSOI grade, injury severity score, hypotension on arrival, and need for transfusions. We performed subset analyses in patients with isolated spleen, kidney, and liver injury. RESULTS: From 1022 cases, 417 (40.8%) adolescents received eVTEP. After matching, there was no difference in matched variables (all p > 0.05). Both groups had a similar rate of VTE (dVTEP 0.6% vs. eVTEP 1.7%, p = 0.16), mortality (dVTEP 0.3% vs. eVTEP 0%, p = 0.32), and failure of NOM (eVTEP 6.7% vs. dVTEP 7.3%, p = 0.77). These findings remained true in all subset analyses of isolated solid organ injury (all p > 0.05). CONCLUSIONS: The rate of VTE with adolescent BSOI is exceedingly rare. Early VTE chemoprophylaxis in adolescent BSOI does not increase the rate of failing NOM. However, unlike adult trauma patients, adolescent patients with BSOI receiving eVTEP had a similar rate of VTE and death, compared to adolescents receiving dVTEP.

Published
2024

80. Single-Cell Spatial Transcriptomics Unveils Platelet-Fueled Cycling Macrophages for Kidney Fibrosis.

Author

Liu, Jun, Zheng, Bo, Cui, Qingya, Zhu, Yu, Chu, Likai, Geng, Zhi, Mao, Yiming, Wan, Lin, Cao, Xu, Xiong, Qianwei, Guo, Fujia, Yang, David, Hsu, Ssu-Wei, Chen, Ching-Hsien, and Yan, Xiangming

Subjects
kidney fibrosis, macrophage proliferation, platelet, thrombospondin 1, Macrophages, Animals, Fibrosis, Mice, Blood Platelets, Transcriptome, Disease Models, Animal, Male, Mice, Inbred C57BL, Acute Kidney Injury, Single-Cell Analysis, Reperfusion Injury, Kidney
Abstract

With the increasing incidence of kidney diseases, there is an urgent need to develop therapeutic strategies to combat post-injury fibrosis. Immune cells, including platelets, play a pivotal role in this repair process, primarily through their released cytokines. However, the specific role of platelets in kidney injury and subsequent repair remains underexplored. Here, the detrimental role of platelets in renal recovery following ischemia/reperfusion injury and its contribution to acute kidney injury  to chronic kidney disease transition is aimed to investigated. In this study, it is shown that depleting platelets accelerates injury resolution and significantly reduces fibrosis. Employing advanced single-cell and spatial transcriptomic techniques, macrophages as the primary mediators modulated by platelet signals is identified. A novel subset of macrophages, termed cycling M2, which exhibit an M2 phenotype combined with enhanced proliferative activity is uncovered. This subset emerges in the injured kidney during the resolution phase and is modulated by platelet-derived thrombospondin 1 (THBS1) signaling, acquiring profibrotic characteristics. Conversely, targeted inhibition of THBS1 markedly downregulates the cycling M2 macrophage, thereby mitigating fibrotic progression. Overall, this findings highlight the adverse role of platelet THBS1-boosted cycling M2 macrophages in renal injury repair and suggest platelet THBS1 as a promising therapeutic target for alleviating inflammation and kidney fibrosis.

Published
2024

81. Cilia-enriched oxysterol 7β,27-DHC is required for polycystin ion channel activation.

Author

Ha, Kodaji, Mundt-Machado, Nadine, Bisignano, Paola, Pinedo, Aide, Raleigh, David, Loeb, Gabriel, Reiter, Jeremy, Cao, Erhu, and Delling, Markus

Subjects
Cilia, TRPP Cation Channels, Animals, Humans, Polycystic Kidney, Autosomal Dominant, Oxysterols, Patch-Clamp Techniques, HEK293 Cells, Mutation, Kidney, Mice, Binding Sites
Abstract

Polycystin-1 (PC-1) and PC-2 form a heteromeric ion channel complex that is abundantly expressed in primary cilia of renal epithelial cells. This complex functions as a non-selective cation channel, and mutations within the polycystin complex cause autosomal dominant polycystic kidney disease (ADPKD). The spatial and temporal regulation of the polycystin complex within the ciliary membrane remains poorly understood. Using both whole-cell and ciliary patch-clamp recordings, we identify a cilia-enriched oxysterol, 7β,27-dihydroxycholesterol (DHC), that serves as a necessary activator of the polycystin complex. We further identify an oxysterol-binding pocket within PC-2 and showed that mutations within this binding pocket disrupt 7β,27-DHC-dependent polycystin activation. Pharmacologic and genetic inhibition of oxysterol synthesis reduces channel activity in primary cilia. In summary, our findings reveal a regulator of the polycystin complex. This oxysterol-binding pocket in PC-2 may provide a specific target for potential ADPKD therapeutics.

Published
2024

82. Comparison of estimated GFR using cystatin C versus creatinine in pediatric kidney transplant recipients.

Author

Pizzo, Helen, Nguyen, John, Schwartz, George, Wesseling-Perry, Katherine, Ettenger, Robert, Chambers, Eileen, and Weng, Patricia

Subjects
Accuracy, Bias, Estimating equations, Kidney function, Precision, Humans, Cystatin C, Glomerular Filtration Rate, Child, Male, Female, Kidney Transplantation, Creatinine, Adolescent, Child, Preschool, Infant, Iohexol, Renal Insufficiency, Chronic, Kidney, Biomarkers, Transplant Recipients
Abstract

BACKGROUND: An accurate, rapid estimate of glomerular filtration rate (GFR) in kidney transplant patients affords early detection of transplant deterioration and timely intervention. This study compared the performance of serum creatinine (Cr) and cystatin C (CysC)-based GFR equations to measured GFR (mGFR) using iohexol among pediatric kidney transplant recipients. METHODS: CysC, Cr, and mGFR were obtained from 45 kidney transplant patients, 1-18 years old. Cr- and CysC-estimated GFR (eGFR) was compared against mGFR using the Cr-based (Bedside Schwartz, U25-Cr), CysC-based (Gentian CysC, CAPA, U25-CysC), and Cr-CysC combination (CKiD Cr-CysC, U25 Cr-CysC) equations in terms of bias, precision, and accuracy. Bland-Altman plots assessed the agreement between eGFR and mGFR. Secondary analyses evaluated the formulas in patients with biopsy-proven histological changes, and K/DOQI CKD staging. RESULTS: Bias was small with Gentian CysC (0.1 ml/min/1.73 m2); 88.9% and 37.8% of U25-CysC estimations were within 30% and 10% of mGFR, respectively. In subjects with histological changes on biopsy, Gentian CysC had a small bias and U25-CysC were more accurate-both with 83.3% of and 41.7% of estimates within 30% and 10% mGFR, respectively. Precision was better with U25-CysC, CKiD Cr-CysC, and U25 Cr-CysC. Bland-Altman plots showed the Bedside Schwartz, Gentian CysC, CAPA, and U25-CysC tend to overestimate GFR when > 100 ml/min/1.72 m2. CAPA misclassified CKD stage the least (whole cohort 24.4%, histological changes on biopsy 33.3%). CONCLUSIONS: In this small cohort, CysC-based equations with or without Cr may have better bias, precision, and accuracy in predicting GFR.

Published
2024

83. Residual Kidney Function in Hemodialysis: Its Importance and Contribution to Improved Patient Outcomes.

Author

Obi, Yoshitsugu, Raimann, Jochen, Kalantar-Zadeh, Kamyar, and Murea, Mariana

Subjects
incremental hemodialysis, randomized controlled trial, residual kidney function, Renal Dialysis, Humans, Kidney, Treatment Outcome
Abstract

Individuals afflicted with advanced kidney dysfunction who require dialysis for medical management exhibit different degrees of native kidney function, called residual kidney function (RKF), ranging from nil to appreciable levels. The primary focus of this manuscript is to delve into the concept of RKF, a pivotal yet under-represented topic in nephrology. To begin, we unpack the definition and intrinsic nature of RKF. We then juxtapose the efficiency of RKF against that of hemodialysis in preserving homeostatic equilibrium and facilitating physiological functions. Given the complex interplay of RKF and overall patient health, we shed light on the extent of its influence on patient outcomes, particularly in those living with advanced kidney dysfunction and on dialysis. This manuscript subsequently presents methodologies and measures to assess RKF, concluding with the potential benefits of targeted interventions aimed at preserving RKF.

Published
2024

86. Extensive evaluation of a new LC–MS-MS method to quantify monofluoroacetate toxin in the kidney

Author

Langston, James, Stump, Samuel, Filigenzi, Michael, Tkachenko, Andriy, Guag, Jake, Poppenga, Robert, and Rumbeiha, Wilson K

Subjects
Analytical Chemistry, Biomedical and Clinical Sciences, Chemical Sciences, Tandem Mass Spectrometry, Fluoroacetates, Animals, Kidney, Chromatography, Liquid, Limit of Detection, Reproducibility of Results, Liquid Chromatography-Mass Spectrometry, Pharmacology and Pharmaceutical Sciences, Pharmacology and pharmaceutical sciences, Analytical chemistry
Abstract

Monofluoroacetate is a highly lethal toxin that causes death by inhibiting cellular adenosine triphosphate (ATP) production. The heart and brain are the primary target organs. Acute death is attributed to cardiac fibrillation and/or convulsions. Although it occurs naturally in some plants, a major source of animal intoxication is access to sodium monofluoroacetate (NaMFA) pesticide, which continues to be a concern in the USA and around the world despite restricted use in some countries including the USA. There are also concerns about misuse of this pesticide for malicious poisoning. Currently, a tissue-based diagnostic method for NaMFA intoxication in animals is lacking. There is a critical need by the veterinary diagnostic community for a simple, sensitive and reliable tissue-based diagnostic test to confirm NaMFA poisoning in animals. We have developed and extensively evaluated a sensitive novel liquid chromatography combined with tandem mass spectrometry method suitable for this purpose. The limits of detection and limits of quantitation are 1.7 and 5.0 ng/g, respectively. The accuracy and precision met or exceeded expectations. The method performance was verified using the incurred kidney obtained from animal diagnostic cases. This novel kidney-based method is now available for clinical use and can help with diagnostic purposes, including detecting potential issues related to animal foods.

Published
2024

87. Management of pediatric renal trauma: Results from the American Association for Surgery and Trauma Multi-Institutional Pediatric Acute Renal Trauma Study

Author

Hwang, Catalina K, Matta, Rano, Woolstenhulme, Jonathan, Britt, Alexandra K, Schaeffer, Anthony J, Zakaluzny, Scott A, Kleber, Kara Teresa, Sheikali, Adam, Flynn-O'Brien, Katherine T, Sandilos, Georgianna, Shimonovich, Shachar, Fox, Nicole, Hess, Alexis B, Zeller, Kristen A, Koberlein, George C, Levy, Brittany E, Draus, John M, Sacks, Marla, Chen, Catherine, Luo-Owen, Xian, Stephens, Jacob Robert, Shah, Mit, Burks, Frank, Moses, Rachel A, Rezaee, Michael E, Vemulakonda, Vijaya M, Halstead, N Valeska, LaCouture, Hunter M, Nabavizadeh, Behnam, Copp, Hillary, Breyer, Benjamin, Schwartz, Ian, Feia, Kendall, Pagliara, Travis, Shi, Jennifer, Neuville, Paul, and Hagedorn, Judith C

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Kidney Disease, Pediatric, Physical Injury - Accidents and Adverse Effects, 7.3 Management and decision making, Injuries and accidents, Humans, Male, Female, Child, Retrospective Studies, United States, Kidney, Injury Severity Score, Trauma Centers, Adolescent, Wounds, Nonpenetrating, Child, Preschool, Infant, Multi-institutional, pediatric trauma, renal trauma, trauma centers, conservative management, Clinical sciences, Nursing
Abstract

BackgroundPediatric renal trauma is rare and lacks sufficient population-specific data to generate evidence-based management guidelines. A nonoperative approach is preferred and has been shown to be safe. However, bleeding risk assessment and management of collecting system injury are not well understood. We introduce the Multi-institutional Pediatric Acute Renal Trauma Study (Mi-PARTS), a retrospective cohort study designed to address these questions. This article describes the demographics and contemporary management of pediatric renal trauma at Level I trauma centers in the United States.MethodsRetrospective data were collected at 13 participating Level I trauma centers on pediatric patients presenting with renal trauma between 2010 and 2019. Data were gathered on demographics, injury characteristics, management, and short-term outcomes. Descriptive statistics were used to report on demographics, acute management, and outcomes.ResultsIn total, 1,216 cases were included in this study. Of all patients, 67.2% were male, and 93.8% had a blunt injury mechanism. In addition, 29.3% had isolated renal injuries, and 65.6% were high-grade (American Association for the Surgery of Trauma Grades III-V) injuries. The mean Injury Severity Score was 20.5. Most patients were managed nonoperatively (86.4%), and 3.9% had an open surgical intervention, including 2.7% having nephrectomy. Angioembolization was performed in 0.9%. Collecting system intervention was performed in 7.9%. Overall mortality was 3.3% and was only observed in patients with multiple injuries. The rate of avoidable transfer was 28.2%.ConclusionThe management and outcomes of pediatric renal trauma lack data to inform evidence-based guidelines. Nonoperative management of bleeding following renal injury is a well-established practice. Intervention for renal trauma is rare. Our findings reinforce differences from the adult population and highlights opportunities for further investigation. With data made available through Mi-PARTS, we aimed to answer pediatric specific questions, including a pediatric-specific bleeding risk nomogram, and better understanding indications for interventions for collecting system injuries.Level of evidencePrognostic and Epidemiological; Level IV.

Published
2024

88. Novel indications for referral and care for simultaneous liver kidney transplant recipients.

Author

Bunnapradist, Suphamai, Wiseman, Alexander, Gurakar, Ahmet, Ferrey, Antoney, Reddy, Uttam, Al Ammary, Fawaz, and Lum, Erik

Subjects
Humans, Kidney Transplantation, Renal Dialysis, Risk Factors, Kidney, Renal Insufficiency, Graft Survival, Liver, Referral and Consultation, Renal Insufficiency, Chronic
Abstract

PURPOSE OF REVIEW: Kidney dysfunction is challenging in liver transplant candidates to determine whether it is reversible or not. This review focuses on the pertinent data on how to best approach liver transplant candidates with kidney dysfunction in the current era after implementing the simultaneous liver kidney (SLK) allocation policy and safety net. RECENT FINDINGS: The implementation of the SLK policy inverted the steady rise in SLK transplants and improved the utilization of high-quality kidneys. Access to kidney transplantation following liver transplant alone (LTA) increased with favorable outcomes. Estimating GFR in liver transplant candidates remains challenging, and innovative methods are needed. SLK provided superior patient and graft survival compared to LTA only for patients with advanced CKD and dialysis at least 3 months. SLK can provide immunological protection against kidney rejection in highly sensitized candidates. Post-SLK transplant care is complex, with an increased risk of complications and hospitalization. SUMMARY: The SLK policy improved kidney access and utilization. Transplant centers are encouraged, under the safety net, to reserve SLK for liver transplant candidates with advanced CKD or dialysis at least 3 months while allowing lower thresholds for highly sensitized patients. Herein, we propose a practical approach to liver transplant candidates with kidney dysfunction.

Published
2024

89. Computational pathology model to assess acute and chronic transformations of the tubulointerstitial compartment in renal allograft biopsies.

Author

Augulis, Renaldas, Rasmusson, Allan, Laurinaviciene, Aida, Jen, Kuang-Yu, and Laurinavicius, Arvydas

Subjects
Deep learning, Digital image analysis, Digital pathology, Kidney, Machine learning, Morphometry, Multivariate analysis, Nephropathology, Humans, Kidney Transplantation, Reproducibility of Results, Kidney, Biopsy, Allografts
Abstract

Managing patients with kidney allografts largely depends on biopsy diagnosis which is based on semiquantitative assessments of rejection features and extent of acute and chronic changes within the renal parenchyma. Current methods lack reproducibility while digital image data-driven computational models enable comprehensive and quantitative assays. In this study we aimed to develop a computational method for automated assessment of histopathology transformations within the tubulointerstitial compartment of the renal cortex. Whole slide images of modified Picrosirius red-stained biopsy slides were used for the training (n = 852) and both internal (n = 172) and external (n = 94) tests datasets. The pipeline utilizes deep learning segmentations of renal tubules, interstitium, and peritubular capillaries from which morphometry features were extracted. Seven indicators were selected for exploring the intrinsic spatial interactions within the tubulointerstitial compartment. A principal component analysis revealed two independent factors which can be interpreted as representing chronic and acute tubulointerstitial injury. A K-means clustering classified biopsies according to potential phenotypes of combined acute and chronic transformations of various degrees. We conclude that multivariate analyses of tubulointerstitial morphometry transformations enable extraction of and quantification of acute and chronic components of injury. The method is developed for renal allograft biopsies; however, the principle can be applied more broadly for kidney pathology assessment.

Published
2024

90. The Link between Autosomal Dominant Polycystic Kidney Disease and Chromosomal Instability: Exploring the Relationship.

Author

Chen, Chi-Fen, Lin, Hugo, Riley, Daniel, Chen, Yumay, and Chen, Phang-Lang

Subjects
ADPKD, ATM, CHK1, CHK2, DNA damage repair, PKD1, PKD2, checkpoint, Humans, Polycystic Kidney, Autosomal Dominant, TRPP Cation Channels, Mutation, Kidney, Cysts, Chromosomal Instability
Abstract

In autosomal dominant polycystic kidney disease (ADPKD) with germline mutations in a PKD1 or PKD2 gene, innumerable cysts develop from tubules, and renal function deteriorates. Second-hit somatic mutations and renal tubular epithelial (RTE) cell death are crucial features of cyst initiation and disease progression. Here, we use established RTE lines and primary ADPKD cells with disease-associated PKD1 mutations to investigate genomic instability and DNA damage responses. We found that ADPKD cells suffer severe chromosome breakage, aneuploidy, heightened susceptibility to DNA damage, and delayed checkpoint activation. Immunohistochemical analyses of human kidneys corroborated observations in cultured cells. DNA damage sensors (ATM/ATR) were activated but did not localize at nuclear sites of damaged DNA and did not properly activate downstream transducers (CHK1/CHK2). ADPKD cells also had the ability to transform, as they achieved high saturation density and formed colonies in soft agar. Our studies indicate that defective DNA damage repair pathways and the somatic mutagenesis they cause contribute fundamentally to the pathogenesis of ADPKD. Acquired mutations may alternatively confer proliferative advantages to the clonally expanded cell populations or lead to apoptosis. Further understanding of the molecular details of aberrant DNA damage responses in ADPKD is ongoing and holds promise for targeted therapies.

Published
2024

91. Contemporary and Emerging MRI Strategies for Assessing Kidney Allograft Complications: Arterial Stenosis and Parenchymal Injury, From the AJR Special Series on Imaging of Fibrosis.

Author

Bane, Octavia, Lewis, Sara, Lim, Ruth, Carney, Benjamin, Shah, Amar, and Fananapazir, Ghaneh

Subjects
MRI, allograft, kidney, transplant, Humans, Constriction, Pathologic, Kidney, Fibrosis, Kidney Diseases, Graft Rejection, Allografts, Magnetic Resonance Imaging
Abstract

MRI plays an important role in the evaluation of kidney allografts for vascular complications as well as parenchymal insults. Transplant renal artery stenosis, the most common vascular complication of kidney transplant, can be evaluated by MRA using gadolinium and nongadolinium contrast agents as well as by unenhanced MRA techniques. Parenchymal injury occurs through a variety of pathways, including graft rejection, acute tubular injury, BK polyomavirus infection, drug-induced interstitial nephritis, and pyelonephritis. Investigational MRI techniques have sought to differentiate among these causes of dysfunction as well as to assess the degree of interstitial fibrosis or tubular atrophy (IFTA)-the common end pathway for all of these processes-which is currently evaluated by invasively obtained core biopsies. Some of these MRI sequences have shown promise in not only assessing the cause of parenchymal injury but also assessing IFTA noninvasively. This review describes current clinically used MRI techniques and previews promising investigational MRI techniques for assessing complications of kidney grafts.

Published
2024

92. Wait Time Advantage for Transplant Candidates With HIV Who Accept Kidneys From Donors With HIV Under the HOPE Act.

Author

Motter, Jennifer, Hussain, Sarah, Brown, Diane, Florman, Sander, Rana, Meenakshi, Friedman-Moraco, Rachel, Gilbert, Alexander, Stock, Peter, Mehta, Shikha, Mehta, Sapna, Stosor, Valentina, Elias, Nahel, Pereira, Marcus, Haidar, Ghady, Malinis, Maricar, Morris, Michele, Hand, Jonathan, Aslam, Saima, Schaenman, Joanna, Baddley, John, Small, Catherine, Wojciechowski, David, Santos, Carlos, Blumberg, Emily, Odim, Jonah, Apewokin, Senu, Giorgakis, Emmanouil, Bowring, Mary, Werbel, William, Desai, Niraj, Tobian, Aaron, Segev, Dorry, Massie, Allan, and Durand, Christine

Subjects
Humans, Male, Waiting Lists, Kidney, Tissue Donors, Kidney Transplantation, Living Donors, Transplant Recipients, HIV Infections
Abstract

BACKGROUND: Kidney transplant (KT) candidates with HIV face higher mortality on the waitlist compared with candidates without HIV. Because the HIV Organ Policy Equity (HOPE) Act has expanded the donor pool to allow donors with HIV (D + ), it is crucial to understand whether this has impacted transplant rates for this population. METHODS: Using a linkage between the HOPE in Action trial (NCT03500315) and Scientific Registry of Transplant Recipients, we identified 324 candidates listed for D + kidneys (HOPE) compared with 46 025 candidates not listed for D + kidneys (non-HOPE) at the same centers between April 26, 2018, and May 24, 2022. We characterized KT rate, KT type (D + , false-positive [FP; donor with false-positive HIV testing], D - [donor without HIV], living donor [LD]) and quantified the association between HOPE enrollment and KT rate using multivariable Cox regression with center-level clustering; HOPE was a time-varying exposure. RESULTS: HOPE candidates were more likely male individuals (79% versus 62%), Black (73% versus 35%), and publicly insured (71% versus 52%; P

Published
2024

93. Alterations in the proteomes of HepG2 and IHKE cells inflicted by six selected mycotoxins.

Author

Keuter, Lucas, Fortmann, Marco, Behrens, Matthias, and Humpf, Hans-Ulrich

Subjects
*METABOLITES, *CYTOLOGY, *NUCLEOTIDE synthesis, *LIFE sciences, *NUTRITIONALLY induced diseases, *MYCOTOXINS
Abstract

Toxic fungal secondary metabolites, referred to as mycotoxins, emerge in moldy food and feed and constitute a potent but often underestimated health threat for humans and animals. They are structurally diverse and can cause diseases after dietary intake even in low concentrations. To elucidate cellular responses and identify cellular targets of mycotoxins, a bottom-up proteomics approach was used. We investigated the effects of the mycotoxins aflatoxin B1, ochratoxin A, citrinin, deoxynivalenol, nivalenol and penitrem A on the human hepatoblastoma cell line HepG2 and of ochratoxin A and citrinin on the human kidney epithelial cell line IHKE. Incubations were carried out at sub-cytotoxic concentrations to monitor molecular effects before acute cell death mechanisms predominate. Through these experiments, we were able to detect specific cellular responses that point towards the mycotoxins' mode of action. Besides very well-described mechanisms like the ribotoxicity of the trichothecenes, we observed not yet described effects on different cellular mechanisms. For instance, trichothecenes lowered the apolipoprotein abundance and aflatoxin B1 affected proteins related to inflammation, ribogenesis and mitosis. Ochratoxin A and citrinin upregulated the minichromosomal maintenance complex and nucleotide synthesis in HepG2 and downregulated histones in IHKE. Penitrem A reduced enzyme levels of the sterol biosynthesis. These results will aid in the elucidation of the toxicodynamic properties of this highly relevant class of toxins. [ABSTRACT FROM AUTHOR]

Published
2025
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94. A Rare Tumor of Intravascular Myopericytoma in the Right Renal Vein.

Author

Taniguchi, Kohei, Yanai, Hiroyuki, Honma, Ririno, Yabushita, Hiroki, Yamasaki, Rie, and Ichimura, Koichi

Subjects
*KIDNEY tumors, *HEMANGIOPERICYTOMAS, *BLOOD vessels, *RENAL cancer, *IMMUNOSTAINING, *RENAL veins
Abstract

Myopericytoma, a perivascular myoid neoplasm, is commonly found in the dermis or subcutaneous tissues; however, its occurrence in visceral organs is unusual. Here, we present an extremely rare tumor of intravascular myopericytoma of the right renal vein. A 44-year-old man was incidentally diagnosed with a mass in the right kidney during a routine checkup. A nephrectomy was performed because the urologist suspected renal cancer. A gross examination of the resected specimen revealed a well-circumscribed brown mass in the renal hilum. Histologically, the tumor showed a concentric multilayered proliferation of spindle cells surrounding blood vessels. Immunohistochemical staining showed that the spindle-shaped tumor cells were negative for desmin but positive for α-smooth muscle actin and h-caldesmon, indicating their myoid nature. We confirmed that the tumor was located in the right renal vein because it was encased within a thick wall that was desmin-positive and contained elastic fibers, as shown by Elastica van Gieson staining. The patient was diagnosed with an intravascular myopericytoma of the right renal vein. There are several differential diagnoses for renal mesenchymal tumors, including angiomyolipoma. This emphasizes the importance of considering these uncommon tumors when examining nephrectomy specimens. [ABSTRACT FROM AUTHOR]

Published
2025
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95. Genetic background of neonatal hypokalemia.

Author

Fang, Chuchu and Zhou, Wenhao

Subjects
*INTESTINES, *DIARRHEA, *SKELETAL muscle, *POTASSIUM, *HYPOKALEMIC periodic paralysis, *HYPOKALEMIA, *GENES, *GENETIC mutation, *KIDNEYS, *BARTTER syndrome, *CHILDREN
Abstract

Neonatal hypokalemia (defined as a serum potassium level <3.5 mEq/L) is the most common electrolyte disorder encountered in clinical practice. In addition to common secondary causes, primary genetic etiologies are also closely associated with hypokalemia. Currently, a systematic characterization of these genetic disorders is lacking, making early recognition challenging and clinical management uncertain. This review will aid clinicians by summarizing the genetic background of neonatal hypokalemia from two aspects: (1) increased excretion of K+, whereby genetic factors primarily lead to increased renal Na+ influx, decreased H+ efflux, or reduced Cl− influx, ultimately resulting in increased K+ efflux; and (2) decreased extracellular distribution of K+, whereby genetic factors result in abnormalities in transmembrane ion channels, reducing outward potassium currents or generating inward cation leak currents. We describe over ten genetic diseases associated with neonatal hypokalemia, which involve pathogenic variants in dozens of genes and affect multiple target organs, including the kidneys, intestines, and skeletal muscle. For example, in the renal tubules, pathogenic variants in the SLC12A1 gene encoding the Na+-K+-2Cl- cotransporter lead to renal K+ loss, causing Bartter syndrome type I; in intestinal epithelial cells, pathogenic variants in the SLC26A3 gene result in a defective Cl⁻-HCO₃⁻ exchanger, causing congenital chloride diarrhea; and in skeletal muscle, pathogenic variants in the CACNA1S gene impact membrane calcium ion channels resulting in hypokalemic periodic paralysis. Given the wide variety of organs and genetic alterations that can contribute to neonatal hypokalemia, we believe this review will provide valuable insights for clinical diagnosis and treatment. [ABSTRACT FROM AUTHOR]

Published
2025
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96. Perfluorooctane sulfonate causes HK-2 cell injury through ferroptosis and endoplasmic reticulum stress pathways.

Author

Yan, Shuqi, Ma, Haoyan, Ren, Yuwan, Wang, Pingwei, Liu, Dongge, Ding, Na, Liu, Yanping, Chen, Qianqian, Ren, Shuping, and Mou, Yan

Subjects
*PERFLUOROOCTANE sulfonate, *ENDOPLASMIC reticulum, *IRON ions, *CELL survival, *INDUSTRIAL goods
Abstract

Perfluorooctane sulfonate (PFOS) is a synthetic persistent organic compound that is widely used in industrial products. Studies have shown that PFOS can accumulate in environment and pose a threat to human health. As the kidney is the main excretory organ for PFOS, it is important to study PFOS damage to the kidney to investigate its toxicity. Human proximal tubular epithelial cells (HK-2) were treated with 200 μM PFOS or 1 μM Fer-1. Cell viability, the levels of MDA, GSH, intracellular iron ion, and GPX-4 were determined. The expression of KIM-1 and endoplasmic reticulum stress (ERS) related proteins were determined. The expression levels of KIM-1, a marker of renal tubular injury, and ERS-related proteins, GRP78, ATF6, IRE1, and PERK, were significantly increased in HK-2 cells exposed to PFOS. The levels of MDA and intracellular total iron ion also were significantly increased in HK-2 cells exposed to PFOS and the levels of GSH and GPX-4 were significantly decreased. PFOS can damage HK-2 cells through ferroptosis and endoplasmic reticulum stress, which provides a theoretical foundation for exploring the toxicity of PFOS to the kidney. [ABSTRACT FROM AUTHOR]

Published
2025
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97. Brief Report: Cystatin C Provides Substantially Higher Glomerular Filtration Rate Estimates Than Creatinine in a Subset of Black People With HIV on Current Antiretroviral Regimens.

Author

Dominguez-Dominguez, Lourdes, Hamzah, Lisa, Fox, Julie, Vincent, Royce P., and Post, Frank A.

Abstract

Supplemental Digital Content is Available in the Text. Background: In African populations, estimated glomerular filtration rate by cystatin C (eGFRcys) is better aligned with gold-standard GFR measurements than eGFR by creatinine (eGFRcr). Moreover, eGFRcys is unaffected by the effects of antiretroviral therapy (ART) on tubular secretion and may thus provide better estimates of GFR in people with HIV on ART. Setting: Observational cohort study of people of African ancestry living with suppressed HIV RNA on ART in London, United Kingdom. Methods: Cross-sectional analysis of 360 paired serum creatinine and cystatin C measurements. Participants whose eGFRcys substantially (>10%) exceeded eGFRcr were identified, and factors associated with this outcome were identified in logistic regression analysis. Results: The median age of participants was 52 years, 56% were women, and 82% born in Africa or the Caribbean. The eGFRcys substantially exceeded eGFRcr in 42% of participants in the overall cohort, and in 68% of those with eGFRcr 45–75 mL/min/1.73 m2. In multivariable analysis, a higher eGFRcr was associated with lower odds (0.59 [0.50, 0.68] per 10 mL/min/1.73 m2 increase) of eGFRcys substantially exceeding eGFRcr; a higher BMI was also associated with this outcome, while ART regimens inhibiting tubular secretion of creatinine were not predictive. Of the 22 participants with eGFRcr 45–60 mL/min/1.73 m2, 16 (73%) had eGFRcys >60 mL/min/1.73 m2. Conclusions: We report substantially higher eGFRcys than eGFRcr in a subset of people of African ancestry with suppressed HIV, particularly among those with eGFRcr 45–75 mL/min/1.73 m2. In this population, eGFRcys provides clinically useful information irrespective of ART regimen. [ABSTRACT FROM AUTHOR]

Published
2025
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98. microRNA and Hypertension.

Author

He, Lishu, Liu, Yong, Widlansky, Michael E., Kriegel, Alison J., Qiu, Qiongzi, and Liang, Mingyu

Abstract

Several microRNAs (miRNAs) strongly influence blood pressure and the development of hypertension by modulating vascular, renal, and other physiological mechanisms. In addition, miRNAs may contribute to the genetic regulation of blood pressure. Future research should focus on investigating select miRNAs with potent physiological effects, understanding cellular context–dependent mechanisms conferring specificity to miRNA action, and integrating miRNAs as powerful modulators into the molecular system that underlies the regulation of blood pressure and the development of hypertension. [ABSTRACT FROM AUTHOR]

Published
2025
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99. The Time Has Come: The Case for Initiating Pilot Clinical Trials of Pig Kidney Xenotransplantation.

Author

Cooper, David K.C., Riella, Leonardo V., Kawai, Tatsuo, Fishman, Jay A., Williams, Winfred W., Elias, Nahel, Madsen, Joren C., and Pierson, Richard N.

Abstract

In vitro studies indicate that kidney transplantation from gene-edited pigs in which expression of all 3 of the known glycan xenoantigens has been deleted may be more challenging in nonhuman primates (NHPs) than it will be in human recipients. Furthermore, pig-to-human xenotransplantation offers several other advantages—(1) the patient can communicate with the surgical team; (2) recipient microbiological monitoring and environment will be clinical-grade; and (3) sophisticated graft monitoring and imaging techniques, (4) therapeutic interventions, eg, dialysis, plasmapheresis, and (5) intensive care can be deployed that are not easily available in NHP laboratory models. We suggest, therefore, that progress to develop safe, informative human clinical trials will be accelerated if pilot clinical cases are initiated. The selection of patients for kidney xenotransplantation can include those who are at high risk of dying imminently, for example, those experiencing increasing vascular access challenges with no realistic alternative therapy available, and those who have been accepted onto the waitlist for an allograft, but who are unlikely ever to receive one. Patients with an increased risk of dying include those with (1) age above 60 years, (2) blood groups O or B, and (3) diabetic nephropathy. UNOS data indicate that an average of 25 patients on the kidney waitlist in the United States die or are removed from the list every day (ie, >9000 each year). Given the improved xenograft survival observed in preclinical studies, we suggest that it is time to plan a small pilot clinical trial for healthy dialysis patients who understand the risks and potential benefits of kidney xenotransplantation. [ABSTRACT FROM AUTHOR]

Published
2025
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100. Clinical manifestations, diagnosis and treatment of hereditary fibrinogen Aα-chain renal amyloidosis: one case report and systematic review.

Author

He, Linying, Zhou, Jiahui, Wang, Miner, Chen, Jianxiang, Liu, Chang, Shi, Jiazhen, Rui, Yanxia, and Wu, Henglan

Abstract

Purpose: We reported a confirmed case of Fibrinogen Aa-chain (AFib) amyloidosis and conducted systematic review of the genetic and protein mutation types, clinical manifestations, diagnostic methods and treatment for patients with this disease worldwide. Methods: We reported a case of AFib amyloidosis. Meanwhile, a systematic search was performed using defined terms and updated up to November 2023 in the Wanfang, China National Knowledge Infrastructure, VIP, PubMed, and Web of Science databases to identify reported cases of AFib renal amyloidosis worldwide, according to PRISMA guidelines. Results: A 46-year-old male patient was admitted for more than half a month because of oedematous lower limbs. Renal tissue mass spectrometry suggested an AFib type. Gene detection demonstrated that the patient carried the c.1673del (p.Lys558Argfs*10) locus heterozygous mutation of Fibrinogen Aα-chain gene (FGA). The patient was treated with haemodialysis because of uncontrollable hypertension. This systematic review comprised 46 cases. We found the onset age to be lower in women than in men (P < 0.05). All patients showed incipient symptoms including proteinuria; 10 (21.7%) patients progressed to end-stage renal disease (ESRD) or received renal replacement therapy (including dialysis and kidney transplantation) within 1 year; 18 (39.1%) patients progressed to ESRD or received renal replacement therapy within 1–5 years, and 4 (8.7%) patients did not progress to ESRD or received renal replacement therapy within 5 years. Conclusion: AFib amyloidosis progresses rapidly. The diagnosis of this disease is primarily based on renal biopsy, mass spectrometry, and molecular gene detection. Reducing proteinuria is the main method of treating this disease. Prospero registration number: CRD42024516146. [ABSTRACT FROM AUTHOR]

Published
2025
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