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Cytokines in minimal change nephropathyParry, Robin Geoffrey January 2000 (has links)
No description available.
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Comparative analysis of the PKD1 gene and protein, polycystin-1Hughes, Jim January 1999 (has links)
No description available.
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The role of reactive oxygen and nitrogen species in the immune response of rainbow trout to Renibacterium salmoninarumCampos-Perez, Juan Jose January 1998 (has links)
The role of reactive oxygen and nitrogen intermediates in the immune response of rainbow trout to R.s. was investigated. The early events occurring when the pathogen interacted with trout macrophages were assessed in terms of the respiratory burst elicited. Live R.s. elicited a respiratory burst, which was enhanced by heat-killed microorganism. This phenomenon, though, was not observed using UV-killed bacteria. Both responses were enhanced when a combination of LPS and TNF was used to activate the macrophages prior to contact R.s. Further studies demonstrated that both compounds synergised to enhance superoxide (O2) production, and that this was correlated with the ability to kill the pathogen. Opsonisation of R.s. with serum factors also increased the respiratory burst, but no difference was found between normal serum and heat-inactivated serum. The role of NO in the immune response of rainbow trout is also studied. Though no evidence of NO production was found in vitro, i.p. injection of live R.s. produced higher NO levels in serum as compared to controls. Fish injected with a virulent strain showed higher levels of NO than controls and than fish injected with an avirulent strain and other strains of unknown virulence. Fish vaccinated with killed R.s. and FIA also showed a significant increase in NO levels, but only four days after vaccination, decreasing thereafter, at both doses of vaccine tested. Injected of Brivax II, an attenuated strain of Aeromonas salmonicida, did not produce a significant increase of NO. RT-PCR was used to detect the expression of the iNOS in different tissues of rainbow trout. iNOS expression was seen only in gill and kidney after i.p. injection. iNOS was detected in the gills 6 h after injecting live R.s. and the expression was still present at day 5. iNOS was detected in the kidney 24 h after injection but was switched off at day 3. After bath challenge with the bacterium, iNOS was expressed in gill, gut and kidney, but the expression varied in each fish. No iNOS expression was found in macrophages isolated from challenged fish.
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Proteinuria in HIV seropositive individualsFabian, June 08 May 2009 (has links)
ABSTRACT
This study was designed to screen antiretroviral therapy (ART)-naïve human immunodeficiency
virus (HIV) infected patients for proteinuria, using urine dipsticks, at the HIV outpatient clinic at
Johannesburg Hospital in an attempt to detect and treat early renal disease. In those with
persistent proteinuria, a marker of kidney disease, renal biopsy was performed, ART with and
without angiotensin-converting enzyme inhibitors (ACE-I) was initiated and patients were
followed up for immunological and renal responses. After a minimum period of 12 months, a
repeat biopsy was performed, where possible, to determine whether the histological lesions had
responded to treatment. During urinary screening, proteinuria, leucocyturia and microscopic
haematuria were common. Sterile leucocyturia may be associated with co-morbid sexually
transmitted infection or tuberculosis. In the group that underwent renal biopsy with treatment,
the renal and immunological response, before and after ART was highly statistically significant.
Renal and immunological responses to ART were assessed by reduction in proteinuria with
increased GFR, increased CD4 count with reduction in HIV viral load, respectively. On biopsy,
HIV-associated immune complex disease was more common than HIVAN, a finding that
contradicts international and some local data. Resolution of proteinuria was relatively rapid in
comparison to the histological response to treatment, an effect not previously shown. This is the
first study of its kind, to the author’s knowledge, that prospectively evaluates the effect of ART
with/ ACE-I in ART-naïve HIV infected patients with both clinicopathological and histological
criteria. It has shown unequivocally, that renal disease, particularly if detected and treated early
in HIV infection, is responsive to treatment. These findings suggest screening for early detection
and treatment of HIV-associated renal disease should be mandatory in HIV clinics in South
Africa.
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Clinical and molecular characterisation of autosomal recessive polycystic kidney disease (ARPKD) in Afrikaans familiesLambie, Lindsay Ann 24 August 2010 (has links)
MSc (Med)(Genetic Counselling), Faculty of Health Sciences, University of the Witwatersrand / Autosomal recessive polycystic kidney disease (ARPKD; MIM263200) is a severe recessively
inherited disease of the kidneys and biliary tract, with an incidence of approximately 1 in
20000 in non-isolated populations. It has a variable clinical spectrum from neonatal demise (in
30-50%) to survival into adulthood. ARPKD is caused by mutations at a single locus,
polycystic kidney and hepatic disease 1 (PKHD1), with over 270 pathogenic mutations
described to date. The high rate of compound heterozygosity in affected individuals has made
genotype-phenotype correlations difficult. A common missense mutation, p.M627K, in exon
20 of PKHD1 was identified previously on the majority of ARPKD disease associated alleles
in the Afrikaans population of South Africa suggesting the presence of a founder effect.
The aim of this study was to describe the clinical phenotype of ARPKD in Afrikaans speaking
individuals found to be homozygous for the common mutation, and to compare this phenotype
to previously described cohorts of patients with ARPKD, known to harbour a spectrum of
mutations. This descriptive study used retrospective data collected from records of patients
with ARPKD at Johannesburg and Pretoria Academic Hospitals. Twenty seven individuals
from 24 families were included in the study.
Marked clinical variability was demonstrated within this subject group supporting the
limitation of genotype-phenotype correlation described worldwide. ARPKD was diagnosed at
a median age of 27 days, older than a North American cohort (NAC) born after 1990 (median
age of 1 day). The majority (93%) of subjects in this study were diagnosed with chronic renal
v
insufficiency (CRI) and hypertension (HT), indicating the renal morbidities to be more
common than noted in previous studies, but occurring at a later median age (1.4 years vs 13.5
days in the NAC). This may indicate a trend toward milder expression of renal morbidities in
the present study. Portal hypertension was also diagnosed more frequently (81%) than in
previous studies but at a younger median age (1.3 years vs 2.8 years), although with similar
complication rates. Overall statistical correlation was found between the renal and hepatic
related morbidities in this study, indicating that progression of the condition is not organ
specific. A survival rate of 89% at one year is comparable to previous studies with similar
patient ascertainment.
This cohort represents the largest series of patients affected by ARPKD with a common
mutation, described to date. The findings will provide for more accurate, specific and
informative genetic counselling in families with ARPKD and may present a resource for
future studies of modifier genes and environmental influences on the phenotypic expression of
ARPKD.
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Reducing acute kidney injury in patients with chronic kidney disease undergoing cardiac surgeryGallagher, Sean January 2014 (has links)
Patients with chronic kidney disease (CKD) are a group with a markedly increased risk of adverse events following cardiac surgery. A particular problem for these patients is the development of post-operative acute kidney injury (AKI), which is associated with a significant increase in morbidity and mortality. Currently, there are no effective therapies proven to modify AKI in patients undergoing cardiac surgery. This thesis has three parts. The first describes an analysis of the Barts Health NHS Trust cardiac surgical dataset. Specifically, outcomes of patients with CKD and AKI were examined. The second describes a randomized control trial that examined the effect of remote ischaemic preconditioning (RIPC) upon AKI and myocardial injury in patients with CKD undergoing coronary artery bypass graft surgery (CABG). The final part describes the development of a panel of AKI biomarkers to allow the accurate prediction of AKI in patients with CKD undergoing CABG. The aims of this thesis were: 1. In our local cardiac surgical cohort, a. To assess the effects of CKD upon outcomes after CABG. b. To asses the prognostic importance of AKI after CABG. 2. To assess the potential for RIPC to reduce AKI and myocardial injury in patients with CKD undergoing CABG. 3. To investigate the diagnostic performance of serum and urine AKI biomarkers in a population of patients with CKD undergoing CABG. Analysis of the Barts Health NHS Trust cardiac surgical dataset confirmed that patients with CKD account for almost one-third of patients undergoing CABG. However, these patients account for a disproportionate two-thirds of all early mortality. CKD was also independently associated with late mortality after CABG. AKI was common in these patients. AKI was associated with late mortality even after accounting for pre-operative comorbidity and surgical complexity. In the randomized control trial, RIPC showed no effect upon the incidence of AKI or myocardial injury in the. 86 patients with CKD recruited. Secondary analysis of serum and urine biomarkers collected found change in serum cystatin C and NGAL as impressive predictors of AKI in patients with CKD. They allowed accurate early prediction of AKI more than 24 hours before diagnosis was possible using serum creatinine.
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The role of indoxyl sulfate in the increased incidence of thrombosis formation in chronic kidney diseaseAlousi, Faisal Fahd 01 November 2017 (has links)
The increased risk of atherothrombosis in chronic kidney disease (CKD) has been under extensive examination for decades now. However, a treatment tailored for CKD patients is yet to be found. Current management plans can only tackle comorbidities and mostly fail. This thesis study examines the current literature related to CKD and thrombosis. The aim is to find a target suitable for therapeutic exploration. Normalizing the risk of thrombosis in CKD patients could curb a huge margin of their morbidity and mortality. In recent years, molecular biology studies attributed the extreme thrombogenicity in CKD to the retained uremic toxins. Indolic compounds are uremic toxins with a well described point of thrombotic activation. Of them, indoxyl sulfate is to be highlighted since it was shown to that it is one of the strongest pro-thrombotic uremic toxin. It is possible to therapeutically target this CKD specific cause of hyperthrombogenicity. Further research is very much needed in this area.
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Association of Age, Gender and Race in Chronic Kidney Disease Patients with and without DialysisOnatolu, Busayo, Zheng, Shimin, Panchal, Hemang, Leinaar, Edward 12 April 2019 (has links)
ASSOCIATION OF AGE, GENDER AND RACE IN CHRONIC KIDNEY DISEASE PATIENTS WITH AND WITHOUT DIALYSIS
1Busayo Adeyemi Onatolu, 2Hemang Panchal, 3Edward Francis Leinaar, 1*Shimin Zheng, 2Timir K. Paul
1Department of Biostatistics and Epidemiology, College of Public Health, ETSU, Johnson City, TN 37614
2Department of Internal Medicine, Quillen College of Medicine, ETSU, Johnson City, TN, 37614
3Department of Health Services Management and Policy, CPH, ETSU, Johnson City, TN 37614
*Sponsoring faculty
Introduction:
Studies have shown that chronic kidney disease (CKD) is common among adults in the United States. The Centers for Disease Control and Prevention (CDC) states that 30 million people, or 15% of US adults, are estimated to have CKD. Forty-eight percent of those with severely reduced kidney function are not aware of having CKD, and therefore do not receive hemodialysis (HD).
Methods:
A nationwide inpatient sample database from 2012-2014 was used to identify all patients admitted to the hospital using International Classification of Diseases, Ninth Revision, Clinical Modification (ICD-9-CM) codes (n= 534,845). Patients with dialysis dependent CKD (n=8,100) and CKD without dialysis (n=51,285) were compared to non-CKD patients (n=475,460). Hierarchical logistic regression was performed and p
Results:
Of the 534,845 patients, 88.9% were without CKD and 9.59% had CKD without HD and 1.51% had CKD with HD. Among patients with CKD, 13.64% were on HD and 86.34% were non-HD patients. The result shows that a higher proportion of patients with CKD without HD in the ≥ 80 years age group (≥ 80 = 37.84%, 65-79 = 36.94%, 50-64 = 20.80%, 35-49 = 4.12% and 18-34 = 0.30%) and a higher proportion of patients with CKD with HD in the 65-79 years age (≥ 80 = 16.30%, 65-79 = 41.79%, 50-64 = 33.09%, 35-64 = 8.09% and 18-34 = 1.29%). The OR of age group 18-34 compared to ≥ 80 is 5.690, 95% CI: 4.202,7.705, OR 35-49 is 4.552, 95% CI: 4.552, 95% CI: 4.103, 5.050, OR of 50-64 is 3.693, 95% CI: 3.444, 3.961 and OR 65-79 is 2.626, 95% CI: 2.457, 2.807. Males had higher rates of CKD than females, without HD (Male= 63.12%, female= 36.88%, p
Conclusion:
From this study, males had higher rates of CKD with and without HD than females, the age group ≥ 80 years had higher proportion of CKD without HD and those between 65-79 years had higher number of CKD with HD. Whites had higher rates of CKD with and without HD than other races.
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Towards consumer-centred health care and health research in nephrology: understanding patient and family caregiver experiences and perspectives in chronic kidney diseaseTong, Allison January 2008 (has links)
Doctor of Philosophy (PhD) / Healthcare services and health research aim to improve the physical and psychosocial well being of consumers, and to offer responsive services needed and valued by them. Research in chronic kidney disease (CKD) has predominantly focused on investigating biomedical aspects and evaluating technological or pharmacological treatment interventions to improve medical management. While research into assessing patients’ and caregivers’ quality of life, and symptom burden, is growing minimal attention has been given to gaining a broad and in-depth understanding about the experiences, psychosocial issues and needs of patients and their caregivers. These need to be considered when planning and delivering patient-centred care and health research across the whole trajectory of CKD. The studies that form the major part of this thesis explore the perspectives, needs and experiences of CKD patients and their caregivers, within a broad and multidimensional framework encompassing aspects of the nature of the health and illness experiences and consumer perspectives. In Chapter 2, to understand what is known about parental experiences of caring for a child with CKD, the relevant qualitative literature was systematically reviewed and synthesized. Three inter-related clusters were identified: intrapersonal, interpersonal and external experiences. In Chapter 3, to gain a more detailed and broader understanding of this topic, in-depth interviews were conducted with parents of 20 children with CKD and 4 major themes were identified: absorbing the clinical environment, medicalising parenting, disrupting family norms, and coping strategies and support structures. In Chapter 4, to assess the effectiveness of support interventions for caregivers of patients with CKD, a systematic review was conducted which identified only three eligible studies that assessed only the effect of educational material on caregiver knowledge, not other domains. In Chapter 5, to describe and compare the broad range and depth of experiences and perspectives from predialysis, dialysis and transplantation patients, data from patient focus groups were analysed. The 5 themes that emerged from this data were: personal meaning of CKD, managing and monitoring health, lifestyle consequences, family impact, and informal structures. In Chapter 6, the focus groups were also used to elicit research priorities and identify reasons that patients used to develop their research priorities. A patient focused research agenda was elicited for CKD and 5 reasons that patients used to develop their research priorities were identified: normalisation of life, altruism, economic efficiency, personal concerns and clinical outcomes. During the focus groups, participants repeatedly expressed frustration about the poor public profile, and lack of community-based information on CKD prevention. So in Chapter 7, to assess how Australian news media covered prevention and early detection of CKD, I analysed television and newspaper stories that referred to CKD prevention or early detection. Kidney disease in general, and particularly the prevention and early detection of CKD, received virtually no media attention. When mentioned, it was mainly in the context of transplantation and donor stories, and seldom prevention or early detection, which appears largely unnewsworthy in its current form. At best, CKD received peripheral mention as a secondary concern in diabetes and obesity news stories which focused on lifestyle solutions. In Chapter 8, to develop a checklist for explicit and comprehensive reporting of qualitative studies (in-depth interviews and focus groups), I performed a comprehensive search in relevant publications for existing checklists used to assess qualitative studies. Seventy-six items from 22 checklists were compiled into a comprehensive list. All items were grouped into three domains: 1) research team and reflexivity, 2) study design, and 3) data analysis and reporting. The overarching purpose of these studies was to gain a better understanding about the needs, experiences and perspectives of CKD patients and their caregivers. The findings describe the permanent, profound and pervasive impact of CKD on the lives of patients and caregivers across the whole illness trajectory. A more detailed and broader understanding about patient and caregiver perspectives, as presented in this thesis, can support a move towards advancing patient-centred healthcare and research in CKD.
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Characterization of candidate genes in English cocker spaniel hereditary nephritisCamacho, Zenaido 17 February 2005 (has links)
Six different isoforms of Type IV collagen (colIVα1-6) have been identified. The individual isoforms of colIV are termed alpha chains and are translated from six different COLIV genes (COLIVA1-A6). Collagen Type IV gene products compose the structural framework of basement membranes. The glomerular basement membrane (GBM) is a specialized basement membrane involved in the ultrafiltration processes of the kidney. The colIVα1-α5 chains are expressed in the human GBM while the colIV α1-α6 chains are expressed in the canine GBM. Many inherited diseases of the kidney have been reported and mutations in genes regulating kidney function have been identified. Alport syndrome (AS) is the most common form of human hereditary nephritis (HN). AS is defined as an inherited progressive kidney disorder associated with sensoneural deafness and is characterized by extensive thickening and multilamminar splitting of the GBM when examined by electron microscopy. AS has both X-linked (XLAS) and autosomal (ARAS) modes of inheritance. Mutations in the COLIVA5 gene are responsible for XLAS. A form of HN with characteristic splitting of the GBM with X-linked inheritance has been described in Samoyed dogs. A specific mutation in the COLIVA5 gene has been identified in Samoyed dogs affected with HN. Mutations in the COLIVA3 and COLIVA4 genes are responsible for ARAS. A form of HN has been identified in English cocker spaniel dogs (ECS) that has been described as autosomal in inheritance and includes GBM abnormalities including extensive lammination characteristic of ARAS. Both ARAS and ECS-HN show loss of the colIVA3 and colIVA4 chains in the GBM when examined with monoclonal anitibodies. ECS-HN has been hypothesized to have the same molecular basis of disease as ARAS. As such, we have isolated and characterized canine COLIVA3 and COLIVA4 sequences from normal dogs and ECS dogs affected with HN and compared the coding regions of these candidate genes.
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