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The Global ETD Search service is a free service for researchers
to find electronic theses and dissertations. This service is
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Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
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Showing 1 to 10 of 22 (0.03 seconds)Spelling suggestions: "subject:"alport"" "subject:"olport""
| 1 |
The clinical and molecular features of hereditary nephritis in Northern IrelandJefferson, Ashley January 1995 (has links)
No description available.
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| 2 |
Genetics of x-linked and autosomal recessive hereditary nephropathy in the domestic dogBell, Rebecca Jane 15 May 2009 (has links)
Although typically thought of as a beloved companion or indispensable aide, the
domestic dog (Canis lupus familiaris) has emerged as an excellent model for the study
of human hereditary diseases. Many hereditary diseases of the dog have nearly identical
clinical presentations as those of the human and are, most often, caused by mutations in
the same genes. One such disease is hereditary nephropathy; an inherited glomerular
disease in the domestic dog that is similar to Alport syndrome of the human. Both
diseases are caused by mutations in the type IV collagens genes, and the disease has
nearly identical pathology and clinical presentations in the dog and human. By studying
this disease in the dog, our laboratory hopes to increase understanding of the disease so
that information that can be applied to both the human and the dog. Reported here is 1)
the development of a genomic based test to determine genotypes of mixed breed dogs in
a colony presenting with X-linked hereditary nephropathy, 2) the determination of
patterns of X-chromosome inactivation in normal dogs and dogs that are carriers of Xlinked
hereditary nephropathy, 3) the design of a synthetic COL4A5 cDNA to be used
for gene therapy treatment of dogs with X-linked hereditary nephropathy, 4) the investigation of type IV collagen gene expression changes in normal dogs and those
affected with X-linked and autosomal recessive hereditary nephropathy, and 5) the
discovery of the mutation causative for autosomal recessive hereditary nephropathy in
the English Cocker Spaniel. Utilization of the colony of dogs affected with X-linked
hereditary nephropathy (for which the causative mutation was previously identified)
allowed for comparisons of type IV collagen gene expression to English Cocker Spaniels
with autosomal recessive hereditary nephropathy. These data were critical to
identification of the gene harboring the causative mutation for autosomal recessive
hereditary nephropathy. Sequencing was performed to identify the mutation. With the
ability to test for carriers of this disease, it is our hope that breeders will use it to to
maintain the desired traits in the ECS while simultaneously eliminating the production of
affected offspring.
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| 3 |
Genetics of X-linked and autosomal recessive hereditary nephropathy in the domestic dogBell, Rebecca Jane 10 October 2008 (has links)
Although typically thought of as a beloved companion or indispensable aide, the
domestic dog (Canis lupus familiaris) has emerged as an excellent model for the study
of human hereditary diseases. Many hereditary diseases of the dog have nearly identical
clinical presentations as those of the human and are, most often, caused by mutations in
the same genes. One such disease is hereditary nephropathy; an inherited glomerular
disease in the domestic dog that is similar to Alport syndrome of the human. Both
diseases are caused by mutations in the type IV collagens genes, and the disease has
nearly identical pathology and clinical presentations in the dog and human. By studying
this disease in the dog, our laboratory hopes to increase understanding of the disease so
that information that can be applied to both the human and the dog. Reported here is 1)
the development of a genomic based test to determine genotypes of mixed breed dogs in
a colony presenting with X-linked hereditary nephropathy, 2) the determination of
patterns of X-chromosome inactivation in normal dogs and dogs that are carriers of X-linked
hereditary nephropathy, 3) the design of a synthetic COL4A5 cDNA to be used
for gene therapy treatment of dogs with X-linked hereditary nephropathy, 4) the investigation of type IV collagen gene expression changes in normal dogs and those
affected with X-linked and autosomal recessive hereditary nephropathy, and 5) the
discovery of the mutation causative for autosomal recessive hereditary nephropathy in
the English Cocker Spaniel. Utilization of the colony of dogs affected with X-linked
hereditary nephropathy (for which the causative mutation was previously identified)
allowed for comparisons of type IV collagen gene expression to English Cocker Spaniels
with autosomal recessive hereditary nephropathy. These data were critical to
identification of the gene harboring the causative mutation for autosomal recessive
hereditary nephropathy. Sequencing was performed to identify the mutation. With the
ability to test for carriers of this disease, it is our hope that breeders will use it to to
maintain the desired traits in the ECS while simultaneously eliminating the production of
affected offspring.
|
| 4 |
Der Einfluss des DDR1+/-/NPHS2+/R140Q-Genotyps auf die Interaktion zwischen glomerulärer Basalmembran und Schlitzmembran im Tiermodell / The Impact of the DDR1+/-/NPHS2+/R140Q-Genotype on the Interaction Between the Glomerular Basement Membrane and the Slit Diaphragm in an Animal ModelSchütte, Peter 20 May 2014 (has links)
No description available.
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| 5 |
Die Bedeutung des Kollagenrezeptors α2β1- Integrin bei der Pathogenese und Prävention der Nierenfibrose in hereditären Typ IV- Kollagen- Erkrankungen / The importance of the collagen- receptor integrin α2β1 in the pathogenesis and prevention of renal fibrosis in hereditary type IV collagen diseasesMartin, Maria 09 May 2011 (has links)
No description available.
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| 6 |
Neue Therapieansätze für das Alport-Syndrom: Nephroprotektives, antifibrotisches und antiinflammatorisches Potential von Paricalcitol additiv zu Ramipril in einem Mausmodell für progressive Nierenfibrose / New therapeutic approaches for the Alport syndromes disease: nephroprotective, antifibrotic and antiinflammatory effects of Paricalcitol on top of Ramipril in a mouse model for progressie renal fibrosisHiller, Henrik 05 August 2014 (has links)
No description available.
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| 7 |
Prospektive Verlaufsstudie über die Auswirkung der RAAS-Blockade bei Trägern des Alport-Syndroms / Prospective follow-up study on the effect of RAAS blockade in carriers of Alport syndromeGlonke, Niklas 11 July 2018 (has links)
No description available.
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| 8 |
Nierenschützende Wirkung von Calcitriol additiv zu Ramipril auf die Nierenfibrose im AlportMaus-Modell / Nephroprotective effects of Calcitriol additive to ramipril on renal fibrosis in Alport miceCiner, Ayse 16 March 2016 (has links)
No description available.
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| 9 |
Präemptive Therapie mit Angiotensin-Converting-Enzyme-Inhibitoren verzögert Nierenersatztherapie bei heterozygoten Mutationsträgerinnen mit X-chromosomalem und autosomal-rezessivem Alport-Syndrom / Pre-emptive treatment with angiotensin converting enzyme inhibitors delays renal replacement therapy in heterozygous carriers of X-chromosomal and autosomal recessive Alport mutationsWüst, Catharina 25 February 2013 (has links)
No description available.
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| 10 |
Prognose von Patienten mit Alport-Syndrom unter Berücksichtigung einer medikamentösen Intervention und verschiedener Nierenersatzverfahren / Prognosis of patients with aport syndrome considering a medical intervention and different renal replacement therapyAssmann, Angela 21 January 2015 (has links)
No description available.
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