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Coronary artery reactivity in diabetes mellitus /Dick, Gregory M. January 1996 (has links)
Thesis (Ph. D.)--University of Missouri--Columbia, 1996. / "December 1996." Typescript. Vita. Includes bibliographical references (leaves 106-117). Also available on the Internet.
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Ca²⁺-desensitization in smooth muscle : from cyclic nucleotides, telokin, to myosin light chain phosphatase /Wu, Xuqiong. January 1998 (has links)
Thesis (Ph. D.)--University of Virginia, 1998. / Includes bibliographical references (p. 105-112). Also available online through Digital Dissertations.
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Oncogenes and second messengers in the regulation of smooth muscle cell growth and differentiationHultgårdh-Nilsson, Anna. January 1991 (has links)
Thesis (doctoral)--Karolinska Institutet, Stockholm, 1991. / Extra t.p. with thesis statement inserted. Includes bibliographical references.
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[Alpha]₂-Macroglobulin and LRP in the regulation of vascular smooth muscle cell physiology /Weaver, Alissa Margaret. January 1997 (has links)
Thesis (Ph. D.)--University of Virginia, 1997. / Spine title: [alpha]₂-M & LRP in atherosclerosis. Includes bibliographical references (180-195). Also available online through Digital Dissertations.
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Cell specific transcriptional regulation of the smooth muscle [alpha]-actin gene promoter : two M-CAT elements have differences in functionalactivity and binding properties in smooth muscle versus non-smooth muscle cells /Swartz, Ellen Ashley. January 1997 (has links)
Thesis (Ph. D.)--University of Virginia, 1997. / Spine title: M-CAT motifs of the SM [alpha]-actin gene. Includes bibliographical references (90-100). Also available online through Digital Dissertations.
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The effect of DHA and EPA on fibrosis-related factors in vascular cellsWhyte, Claire Susan. January 2009 (has links)
Thesis (Ph.D.)--Aberdeen University, 2009. / Title from web page (viewed on July 1, 2009). Includes bibliographical references.
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Cloning, expression and function of Kv11.1 variants in the human jejunum /Farrelly, Angela M. January 2004 (has links)
Thesis (Ph.D.)--University of Nevada, Reno, 2004. / Includes bibliographical references. Online version available on the World Wide Web.
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Efeitos do Ãleo essencial do Eucalyptus tereticornis e dos constituintes 1,8-cineol, α-pineno e β-pineno na motilidade do mÃsculo liso gastrintestinal de ratosDavi Matthews Jucà 26 September 2012 (has links)
Conselho Nacional de Desenvolvimento CientÃfico e TecnolÃgico / O 1,8-cineol, o α-pineno e β-pineno sÃo monoterpenos constituintes do Ãleo essencial de plantas encontradas no Nordeste do Brasil como a âmalva-santaâ e o âeucaliptoâ (Ãleo Essencial do Eucalyptus tereticornis - OEET) que, na medicina popular, sÃo usadas no tratamento de distÃrbios intestinais e respiratÃrios. As aÃÃes miorrelaxantes desses Ãleos essenciais sÃo atribuÃdas à presenÃa desses monoterpenos. Nosso objetivo foi estudar mais detalhadamente os efeitos desses constituintes, assim como o do OEET, sobre a contratilidade do mÃsculo liso gastrintestinal e sobre o efeito procinÃtico em ratos. No presente estudo, foram usados ratos Wistar machos (180-250g) sacrificados por deslocamento cervical. Tiras de duodeno, Ãleo e fundo de estÃmago foram cortados e mantidos em soluÃÃo de Tyrode normal. As contraÃÃes isomÃtricas foram registradas atravÃs de transdutores de forÃa conectados a sistema computadorizado. SoluÃÃes contendo o 1,8-cineol, o α-pineno ou β-pineno foram preparadas em Tween 80 (concentraÃÃo final ≤ 0,2% v/v). Usados isoladamente, o OEET, o 1,8-cineol, o α-pineno e β-pineno diminuÃram o tÃnus basal em tiras de duodeno. Em tÃnus basal de tiras isoladas de fundo gÃstrico, o OEET e o 1,8-cineol possuÃram efeito miorrelaxante, enquanto o α-pineno e o β-pineno possuÃram efeito contrÃtil. Esse efeito contrÃtil do α-pineno e do β-pineno em tiras isoladas de fundo gÃstrico à por possÃvel interferÃncia com o mecanismo dependente de IP3 e independe da ativaÃÃo local do receptor muscarÃnico e de uma aÃÃo central na ativaÃÃo de receptores nicotÃnicos, da mesma forma, o efeito miorrelaxante na musculatura lisa duodenal à mediado por possÃvel interferÃncia com os mecanismos celulares mediados pela formaÃÃo de IP3. AlÃm disso, como demonstrado anteriormente, em Ãleo de rato, esses monoterpenos provavelmente ativam as vias de entrada de Ca2+ para a cÃlula em situaÃÃes de depleÃÃo dos estoques intracelulares. Em estudos de retenÃÃo fracional de corante no trato gastrintestinal, o OEET, o 1,8-cineol, o α-pineno e o β-pineno promoveram a aceleraÃÃo do esvaziamento gÃstrico. O α-pineno e β-pineno tambÃm aceleraram o trÃnsito intestinal e reduziram a complacÃncia gÃstrica. Os nossos dados mostram que OEET possui propriedades prÃ-cinÃticas, que podem ser atribuÃveis aos efeitos contrastantes induzidos por α-pineno e β-pineno, corroborando com dados apresentados anteriormente (JucÃ, 2007). / The monoterpenes 1,8-cineole, α-pinen and β-pinene are constituents commonly found in several essential oils obtained from plants in Brazilian northeast such as âmalva-santaâ and âeucaliptoâ (Essential Oil of Eucalyptus tereticornis - EOET), which are used in folk medicine to treat respiratory and gastrointestinal dysfunctions. Myorelaxant actions are due to the presence of these constituents in their essential oils. The present work aimed to further study the pharmacological effects of these compounds, as well as the EOET, on smooth muscle gastrointestinal contractility and the prokinetic effect in rats. Wistar rats (200-250 g) were used, sacrificed by cervical dislocation. Strips were carefully obtained from gastric fundus, duodenum and ileum, and were maintained in normal Tyrode‟s solution. Isometric contractions were recorded through force transducers coupled to a computerized data acquisition system. Solutions containing 1,8-cineolo, α-pinene or β-pinene were prepared with Tween 80 (final concentration ≤ 0,2% v/v). Solely used, EOET, 1,8-cineole, α-pinene or β-pinene decreased duodenal basal tonus. In basal tone of gastric fundus isolated strips, EOET and 1,8-cineole had relaxant effect, while α-pinene and β-pinene had contractile effect. This contractile effect of α-pinene and β-pinene in isolated strips of gastric fundus is due to possible interference with IP3-dependent mechanism and independent of the muscarinic receptor activation and a central action in the activation of nicotinic receptors, in the same way, the duodenal smooth muscle relaxant effect is mediated by possible interference with the cellular mechanisms mediated by the formation of IP3. Moreover, as shown above, in the rat ileum, monoterpenes activate capacitative Ca2+ entry to intracellular milieu after Ca2+ stores depletion. The α-pinene and β-pinene also accelerated intestinal transit and reduced gastric compliance. Our data show that OEET has prokinetic properties in rats, which may be attributable to the contrasting effects induced by α-pinene and β-pinene, corroborating data presented previously (JucÃ, 2007).
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A study of the relationship of mechanical to electrical activity in smooth muscleAxelsson, J. January 1965 (has links)
No description available.
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Sodium and vascular smooth muscle reactivityRagheb, Mohamed A. January 1973 (has links)
Different drugs which can affect various aspects of sodium transport
were tested on contractile activity of a variety of vascular smooth muscles.
In the rabbit anterior mesenteric-portal vein, diphenylhydantoin sodium (DPH) attenuated the contractile responses to noradrenaline (NA) and the inhibition was reversible by washing. The p-hydroxy derivative, 5-p-hydroxyphenyl)-5-phenylhydantoin (DPHOH), which was reported to lack the anticonvulsant activity and the inhibitory effect of DPH on insulin secretion was without any effect on the rabbit anterior mesenteric vein. The inhibitory effect of DPH on contractile responses to NA was almost abolished by prior treatment with ouabain and in K-free solutions. Evidence
of a Na-Ca interaction is provided by the finding that both low Na and high Ca Krebs attenuates the inhibitory effect of DPH while low Ca Krebs accentuates it.
Electrolyte studies using rat tail arteries showed that DPH could counteract the K loss and Na gain produced by either ouabain containing or K-deficient solutions. Prior cooling of the tissue for one hour at 1° C. and then testing the effect of DPH in K-deficient solutions at 1° C., abolished the ability of DPH to counteract the electrolyte changes in K-deficient solutions.
DPH in normal Krebs solution did not significantly affect the Na content
of rat tail arteries. Under this condition, there was a slight diminution
in the K content.
The results suggest that DPH can stimulate the Na pump in rat tail arteries
under conditions In which Na and Rare going along their electrochemical gradient, and/or under conditions simulating the depolarized state. In normal
Krebs, DPH does not seem to stimulate the Na pump of rat tail arteries. Under such experimental conditions, our data are more suggestive of an inhibition of the Na-K ATPase. Evidence is also provided that the attenuation of contractile responses to NA in the rabbit anterior mesenteric vein, might be related to stimulation of the Na pump.
Further studies were done to outline the effect of alteration of other parameters of Na transport in vascular smooth muscles. Ouabain and ethacrynic acid, both inhibitors of the Na-K ATPase, produced a characteristic pattern of response in the rabbit anterior mesenteric vein. There was at first a contraction, followed by relaxation, which was followed by more persistent contractures at higher doses. The diuretic agent, amiloride, which is reported
to inhibit the passive Na influx in a variety of tissues, was found to attenuate contractile responses to NA in rabbit aortic strips, A.M.V., and rat tail arteries. In aortic strips its effect was specific on the rapid
phase of NA contraction. Since the rapid phase is believed to be the result
f the release of a more tightly bound Ca⁺⁺ pool, the latter effect suggests that amiloride affects mainly the availability of a bound Ca pool to the contractile
protein.
Our results so far suggest that alteration of different parameters of
the Na transport might be involved in altering the amount of ionized Ca⁺⁺ available to the contractile protein. More studies on this subject are needed and might open the way for a better understanding of the Na-Ca interaction in vascular smooth muscles and their possible relation to the hypertensive state. Further experiments were done to study the relaxation of the rabbit anterior mesenteric vein following contractile responses.
It seems that extracellular Na is involved in the relaxation of the rabbit anterior mesenteric vein following contractile responses, since this
tissue, when contracted in low Na solutions, would not relax unless some of the Na is returned to the Krebs solution. Li could not substitute
for Na in this function since the contracture occurred in low Na solutions irrespective of whether the substitute was Tris-HCl or Li. the latter was even more effective than Tris-HCl in inducing contractures
in low Na Krebs. Moreover, relaxation of the rabbit anterior mesenteric vein, following contractile responses to NA was delayed in low Na Krebs irrespective of whether the substitute was Li or Tris-HCl.
Preliminary electron microscopic studies were carried on rabbit anterior mesenteric veins to evaluate the effect of the inhibitors of the ATPase, ethacrynic acid and ouabain, on ultrastructure. Both drugs induced disruption of the myofibrillar structures in doses of 1 mM and 10⁻⁵ M, respectively, when the tissue was exposed to the drug for 2 hours. An impressive finding was the dramatic diminution in the number of plasma-lemmal vesicles in the ethacrynic acid treated tissue. This finding raises the possibility that the formation of these vesicles might be an energy dependent process and opens the way for further studies to evaluate their possible importance in active ionic transport processes. / Medicine, Faculty of / Anesthesiology, Pharmacology and Therapeutics, Department of / Graduate
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