41 |
The Effect of a Disease Management Algorithm and Dedicated Postacute Coronary Syndrome Clinic on Achievement of Guideline ComplianceViswanathan, Sundeep ; Yorio,Jeffrey January 2008 (has links)
Dissertation (Ph.D.) -- University of Texas Southwestern Medical Center at Dallas, 2008. / Vita. Bibliography: p.36-42
|
42 |
Protein prenylation inhibitors reveal a novel role for rhoa and rhoc in trafficking of g protein-coupled receptors through recycling endosomesSalo, Paul David. January 2007 (has links)
Thesis (Ph. D.)--Chemistry and Biochemistry, Georgia Institute of Technology, 2008. / Committee Co-Chair: Hud, Nicholas; Committee Co-Chair: Radhakrishna, Harish; Committee Member: Doyle, Donald; Committee Member: Fahrni, Christoph; Committee Member: McCarty, Nael. Part of the SMARTech Electronic Thesis and Dissertation Collection.
|
43 |
The effect of statins on bone and mineral metabolismMaritz, Frans Jacobus 04 1900 (has links)
Dissertation (PhD)--University of Stellenbosch, 2003. / ENGLISH ABSTRACT: The Effect of Statins on Bone and Mineral Metabolism
Both statins and amino-bisphosphonates reduce the prenylation of proteins which
are involved in cytoskeletal organization and activation of polarized and motile cells.
Consequently statins have been postulated to affect bone metabolism. We investigated
the effects of different doses of simvastatin (1,5,10 and 20mg/Kg/day), administered orally
over 12 weeks to intact female Sprague-Dawley rats, and the effect of simvastatin
20mg/Kg/day in sham and ovariectomised rats, on femoral bone mineral density (BMD)
and quantitative bone histomorphometry (QBH), compared to controls. Similarly, the affect
of atorvastatin (2,5mg/Kg/day) and pravastatin (10mg/Kg/day) on BMD was investigated
and compared to controls. BMD was decreased by simvastatin 1mg/Kg/day (p = 0.042),
atorvastatin (p = 0,0002) and pravastatin (p = 0.002). The effect on QBH parameters
differed with different doses of simvastatin (ANOVA; p = 0.00012). QBH parameters of
both bone formation and resorption were equivalently and markedly increased by
simvastatin 20mg/Kg/day in two independent groups of intact rats, and reflected by a
relatively unchanged BMD. At lower doses, simvastatin 1mg/Kg/day decreased bone
formation while increasing bone resorption as reflected by a marked decrease in BMD.
Ovariectomised animals receiving simvastatin 20mg/Kg/day showed no change in BMD
relative to the untreated ovariectomised controls, their increase in bone formation was
smaller than in sham-operated rats receiving simvastatin and there was no change in
bone resorption. The dose response curves of simvastatin for bone formation and
resorption differed from each other.
From these studies it is concluded that:-
a) low-dose simvastatin (1mg/Kg/day), atorvastatin 2.5mg/Kg/day) and pravastatin
10mg/Kg/day) decrease BMD in rodents;b) 1mg/Kg/day simvastatin decreases bone formation and increases bone
resorption and is reflected by a reduced BMD;
c) 20mg/Kg/day simvastatin increases bone formation and resorption and results
in an unchanged BMD;
d) the effects of simvastatin on QBH differ at different dosages;
e) the dose-response curves for QBH parameters of bone resorption and bone
formation differ from each other;
f) the effects of simvastatin seen in intact rats are not observed in ovariectomised
rats;
g) simvastatin is unable to prevent the bone loss caused by ovariectomy. / AFRIKAANSE OPSOMMING: Die Effek van Statiene op Been en Mineraal Metabolisme
Beide statiene en aminobisfosfonate verminder die prenelasie van proteïene wat
betrokke is in die sitoskeletale organisasie en aktivering van gepolariseerde en
beweeglike selle. Gevolglik is dit gepostuleer dat statiene ‘n invloed sal hê op been
metabolisme. Ons het die effekte van verskillende dossisse van simvastatien (1, 5, 10 en
20mg/Kg/dag), mondelings toegedien oor 12 weke aan intakte vroulike Sprague-Dawley
rotte, en die effek van simvastatien 20mg/Kg/dag op skyn- en ge-ovariektomeerde rotte,
op femorale been mineral digtheid (BMD) en kwantitatiewe been histomorfometrie (KBH),
vergeleke met kontroles, ondersoek. Op ‘n soortgelyke manier is die effek van
atorvastatien (2,5mg/Kg/day) en pravastatien (10mgKg/dag) op BMD ondersoek en
vergelyk met kontroles. BMD is verminder deur simvastatien 1mg/Kg/dag (p = 0.042),
atorvastatien (p = 0.0002) en pravastatien (p = 0.002). Die effekte op KBH parameters het
verskil met verskillende dossisse van simvastatien (ANOVA; p = 0.00012). KBH
parameters van beide been vormasie en resorpsie is vergelykend en merkbaar verhoog
deur simvastatien 20mg/Kg/dag in twee onafhanklike groepe van intakte rotte en is
vergesel deur ‘n relatiewe onveranderde BMD. Met laer dossisse het simvastatien
1mg/Kg/dag been vormasie verminder terwyl been resorpsie verhoog is en is weerspieël
deur ‘n merkbaar verminderde BMD. Ge-ovariektomeerde diere wat simvastatien
20mg/Kg/dag ontvang het, het geen verandering in BMD relatief tot die onbehandelde geovariektomeerde
kontroles getoon nie, en die toename in been vormasie was kleiner as in
die skyngeopereerde rotte wat simvastatien ontvang het en daar was geen verandering in
been resorpsie nie. Die dosis-respons kurwes vir simvastatien vir been vormasie en
resorpsie het van mekaar verskil.
Uit hierdie studies word die volgende gevolgtrekkings gea) lae-dosis simvastatien (1mg/Kg/dag), atorvastatien 2.5mg/Kg/dag en
pravastatien 10mg/Kg/dag verminder BMD in knaagdiere;
b) 1mg/Kg/dag simvastatien verminder been vormasie en verhoog been resorpsie
en veroorsaak gevolglik ‘n velaging in die BMD;
c) 20mg/Kg/dag simvastatien verhoog been vormasie en resorpsie met ‘n
gevolglike onveranderde BMD;
d) die effekte van simvastatien op KBH verskil met verskillende dossisse;
e) die dosis-repons kurwes van been resorpsie en been vormasie veskil van
mekaar
f) die effekte van simvastatien wat waargeneem in intakte rotte word nie gesien in
ge-ovariektomeerde rotte nie;
g) simvastatien kannie die verlies van been wat veroorsaak word deur
ovariektomie voorkom nie.
|
44 |
Cellular electrophysiology of cardiac pacemaker channel-implications on novel drug and gene therapies developmentChan, Yau-chi, 鄭有志 January 2008 (has links)
published_or_final_version / Medicine / Doctoral / Doctor of Philosophy
|
45 |
Cardiovascular effects of Leonotis leonurus extracts in normotensive rats and in isolated perfused rat heart.Obikeze, Kenechukwu January 2004 (has links)
This thesis discussed the cardiovascular effects of the aqueous leaf extract and a fraction of the methanol extract of Leonotis leonurus, a plant commonly used in traditional medicine in South Africa for the treatment of hypertension and other cardiac problems. The cardiovascular effects was tested on anaesthetized normotensive male Wistar rats and isolated perfused rat hearts.
|
46 |
Approaches towards the construction of statin analogues.January 2011 (has links)
Cheung, Chi Yun. / "September 2011." / Thesis (M.Phil.)--Chinese University of Hong Kong, 2011. / Includes bibliographical references (leaves 57-59). / Abstracts in English and Chinese. / Acknowledgment --- p.i / Table of Contents --- p.ii / Abstract --- p.iii / Abstract (Chinese Version) --- p.iv / Abbreviation --- p.v / Chapter 1. --- Introduction --- p.1 / Chapter 1.1 --- General Background --- p.1 / Chapter 1.2 --- Mechanism of action --- p.3 / Chapter 1.2.1 --- Biosynthetic pathway of cholesterol --- p.3 / Chapter 1.2.2 --- Inhibition of HMG-CoA reductase by statins --- p.4 / Chapter 1.2.3 --- Plasma cholesterol reduction effect --- p.5 / Chapter 1.3 --- Previous syntheses of statin analogs --- p.5 / Chapter 1.3.1 --- Synthesis from (S)-malic acid --- p.6 / Chapter 1.3.2 --- Synthesis via enantioselective deprotonation --- p.7 / Chapter 1.3.3 --- Synthesis via asymmetric Diels-Alder reaction --- p.9 / Chapter 2. --- Results and Discussion --- p.11 / Chapter 2.1 --- Approaches towards construction of statin analogs --- p.11 / Chapter 2.2 --- Attempt to synthesize alkene 49 from D-arabinose --- p.12 / Chapter 2.3 --- Construction of alkene 49 from D-mannitol --- p.14 / Chapter 2.4 --- Olefin metathesis and conversion to statin analogs --- p.28 / Chapter 3. --- Conclusion --- p.32 / Chapter 4. --- Experimental Section --- p.33 / Chapter 5. --- References --- p.57 / Chapter 6. --- Appendix ii --- p.60
|
47 |
Development of a high throughput small molecule screen using Staphylococcus aureus invasion of cellsKenney, Shelby R. January 2009 (has links)
Thesis (M.S.)--Ball State University, 2009. / Title from PDF t.p. (viewed on Nov. 30, 2009). Includes bibliographical references (p. 74-80).
|
48 |
THE EFFECT OF BETA-ADRENERGIC BLOCKADE ON THE DRIFT IN OXYGEN CONSUMPTION WITH PROLONGED EXERCISEKalis, Joni Kathryn January 1985 (has links)
No description available.
|
49 |
Protein prenylation inhibitors reveal a novel role for rhoa and rhoc in trafficking of g protein-coupled receptors through recycling endosomesSalo, Paul David 24 August 2007 (has links)
LPA1 lysophosphatidic acid receptors (LPA1Rs) are normally present on the surface of the cell. Our initial findings were that HMG-CoA reductase inhibitors (atorvastatin and mevastatin) induce the sequestration of the G protein-coupled LPA1R in recycling endosomes, most likely by inhibiting the recycling of tonically internalized receptors. Whereas, co-addition of geranylgeranylpyrophosphate (GGPP) or geranylgeraniol (GGOH) prevented atorvastatin-induced sequestration of LPA1Rs, the geranylgeranyltransferase-I inhibitor, GGTI-298, mimicked atorvastatin and induced LPA1R sequestration. This suggested that statin-induced endosomal sequestration was caused by defective protein prenylation. The likely targets of atorvastatin and GGTI-298 are the Rho family GTPases, RhoC and RhoA, since both inhibitors greatly reduced the abundance of these GTPases and since knockdown of endogenous RhoC or RhoA with small interfering RNAs (siRNAs) led to endosomal sequestration of LPA1R. Knockdown of RhoC was much more potent at inducing endosomal sequestration than knockdown of either RhoA or RhoB. In contrast, atorvastatin, GGTI-298, siRNA against RhoA, B, or C did not alter the internalization or recycling of transferrin receptors, indicating that recycling of transferrin receptors is distinct from LPA1Rs. Thus, these results, for the first time, implicate RhoA and RhoC in endocytic recycling of LPA1Rs and identify atorvastatin and GGTI-298 as novel inhibitors of this process. / Per the request of the author and advisor, and with the approval of the Graduate Education office, the following changes were made to this thesis:
Replaced original page 1 with Errata Page 2.
Replaced original pages 3-28 with Errata Pages 3 – 16.
Replaced original pages 69-71 with Errata pages 17 – 19.
|
50 |
The role of phosphoinositide 3-kinase (PI3K) in mediating mitogen and Simvastatin induced effects in the vasculatureLiby, Tiera A. January 2005 (has links)
Statins induce beneficial vascular effects. How statins induce beneficial vascular effects is yet to be determined. Here we examine Simvastatin and vascular endothelial growth factor (VEGF) acting through the phosphoinositide 3-kinase (PI3K) pathway in human coronary artery endothelial cells (HCAEC). While Simvastatin and VEGF both activated mediators in the PI3K pathway, the proteins and the rates of activation were not always consistent. This suggests that although Simvastatin and VEGF share a common PI3K pathway in HCAEC and similar vascular effects, the agonists diverge in the induction of cellular signaling cascades. Simvastatin also was shown to induce phosphoinositide 3, 4, 5-triphosphate (PIPS) organization and PI3K p110 gamma (y) perinuclear localization. Beneficial, non-lipid lowering effects of statins may occur through the PI3K pathway through activation of distinct mediators from those of VEGF. Better understanding of the pathways associated with statins is necessary for the discovery of better treatments for cardiovascular disease (CVD). / Department of Biology
|
Page generated in 0.3538 seconds