Excitation contraction coupling in bladder smooth muscle

膀胱平滑肌的兴奋收缩耦合

• 批准号: 8233937
• 负责人: Robert S Moreland
• 金额: $ 33.27万
• 依托单位: DREXEL UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2010
• 资助国家: 美国
• 起止时间: 2010-03-01 至 2014-02-28
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8233937
• 关键词: Accounting; Affect; Age; Asthma; Basic Science; Behavior; Benign Prostatic Hypertrophy; Birth; Bladder; Bladder Diseases; Calcium; Calcium Channel; Calcium Channel Blockers; Carbachol; Cell Culture Techniques; Child; Complex; Contractile Proteins; Corpora Cavernosa; Coupling; Cyclic GMP; Development; Diet; Dilator; Disease; Disinhibition; Ejaculation; End stage renal failure; Erectile dysfunction; Esthesia; Ethnic Origin; Evaluation; Event; Extravasation; Future; Goals; Incidence; Information Systems; Intracellular Signaling Proteins; Investigation; Kidney; Learning; Life; Medicine; Modeling; Muscle Cells; Muscle Contraction; Myosin Light Chain Kinase; Myosin Light Chains; Myosin Regulatory Light Chains; Nitric Oxide; Obstruction; Organ Culture Techniques; Oryctolagus cuniculus; Pain; Paper; Pathology; Pathway interactions; Patients; Phenotype; Phosphodiesterase Inhibitors; Phosphoric Monoester Hydrolases; Phosphorylation; Physiological; Population Group; Preparation; Prevalence; Progress Review Group; Protein Isoforms; Protein Kinase C; Proteins; Publishing; Quality of life; Regulation; Relaxation; Reporting; Research; Research Design; Rho-associated kinase; Role; Scientist; Series; Signal Pathway; Signal Transduction; Signaling Protein; Small Interfering RNA; Smooth Muscle; Smooth Muscle Myocytes; Stimulus; Stream; Stretching; Study models; Surveys; Symptoms; Targeted Research; Testing; Tissues; Urethra; Urination; Vascular Smooth Muscle; Work; base; caldesmon; design; hypertension treatment; innovation; knock-down; lower urinary tract symptoms; male; men; myosin phosphatase; novel; novel therapeutic intervention; public health relevance; repaired; research study; respiratory smooth muscle; sildenafil; statistics; urinary; urinary tract obstruction; urologic

DESCRIPTION (provided by applicant): The prevalence of benign prostatic hyperplasia (BPH) increases as men age. Although BPH is not life threatening, the symptoms increasingly interfere with the quality of life, with lower urinary tract symptoms such as frequent urination, the sensation of incomplete bladder emptying, interrupted orweak urinary stream, and urinary leakage. One major component of the urinary bladder that is responsible for many aspects of voiding behavior is bladder smooth muscle. Unfortunately our understanding of the regulation of smooth muscle in normal bladder is incomplete which has hampered investigations into the changes that occur during diseased states. Therefore the focus of this proposal is to fill these gaps by developing a detailed mechanisitic understanding of excitation-contraction coupling of bladder smooth muscle. The global hypothesis that this proposal will test is that stimulation of bladder smooth muscle produces activation of signaling pathways leading to contraction as well as modulatory pathways that alter the final level of force produced for a given stimulus. These pathways include primarily the myosin light chain (MLC) kinase, the MLC phosphatase, activated and constitutively active Rho kinases, and protein kinase C (PKC). The specific hypothesis that this proposal will test is that bladder smooth muscle contains a constitutively active stretch dependent Rho kinase that sets the tone on the muscle cells in the unstimulated bladder wall. Stimulation of the bladder smooth muscle then initiates a series of events involving calcium dependent MLC phosphorylation, activated Rho kinase, and PKC which by linear and cross-talk pathways fine tune the levels of force produced via actions on the MLC kinase and phosphatase. The fact that smooth muscles subjected to cell culture phenotypically modulate into a non-muscle phenotype has hampered smooth muscle research. In order to circumvent this problem, we have developed a novel organ-cultured bladder smooth muscle tissue that maintains viability and the contractile phenotype and allows introduction of siRNA. The first aim of this proposal will be to continue the development of this organ-cultured preparation and demonstrate the utility of siRNA knock-down. The second aim will test the hypothesis that protein kinase C is an integral part of the signaling in the regulation of bladder smooth muscle contraction and that specific isoforms of protein kinase C are involved in specific steps in this signaling. We will also test the hypothesis that protein kinase C affects the activity of Rho kinase. The third aim will examine the role of Rho kinase in the regulation of bladder smooth muscle contraction. We will test the hypothesis that a constitutively active, stretch-dependent Rho kinase sets the basal tone in bladder smooth muscle and that a second Rho kinase is involved in the regulation of MLC phosphatase activity. These studies will allow us to develop a detailed, mechanistic model of bladder smooth muscle regulation which we will use to construct studies aimed at understanding the changes in regulation that occur in disease states such as BPH. PUBLIC HEALTH RELEVANCE: This proposal is aimed at understanding how the smooth muscle in the urinary bladder functions. There are several diseases of the bladder that significantly impact quality of life. Unfortunately, we know so little about the regulation of normal bladder that it is difficult to study diseased bladder. The studies proposed in this application will provide this missing information. If we can learn how normal bladder is controlled, we can then design experiments to study and hopefully repair abnormal bladder

描述（由申请人提供）：良性前列腺增生（BPH）的患病率随着男性年龄的增长而增加。虽然BPH不会危及生命，但其症状越来越多地干扰生活质量，下尿路症状如尿频、膀胱排空不完全的感觉、尿流中断或微弱以及尿漏。膀胱平滑肌是膀胱的一个主要组成部分，负责排尿行为的许多方面。不幸的是，我们对正常膀胱平滑肌调节的理解是不完整的，这阻碍了对疾病状态下发生的变化的研究。因此，该建议的重点是通过对膀胱平滑肌兴奋-收缩偶联的详细机制理解来填补这些空白。该提议将测试的总体假设是，刺激膀胱平滑肌产生导致收缩的信号通路的激活以及改变给定刺激产生的力的最终水平的调节通路。这些途径主要包括肌球蛋白轻链（MLC）激酶、MLC磷酸酶、激活的和组成型活性Rho激酶和蛋白激酶C（PKC）。该提议将测试的具体假设是膀胱平滑肌含有组成性活性牵张依赖性Rho激酶，其在未刺激的膀胱壁中对肌细胞设定基调。然后刺激膀胱平滑肌引发一系列事件，涉及钙依赖性MLC磷酸化、活化的Rho激酶和PKC，其通过线性和串扰途径微调经由对MLC激酶和磷酸酶的作用产生的力的水平。经过细胞培养的平滑肌表型调节成非肌肉表型的事实阻碍了平滑肌研究。为了规避这个问题，我们已经开发了一种新的器官培养的膀胱平滑肌组织，保持活力和收缩表型，并允许引入siRNA。该提案的第一个目的是继续开发这种器官培养的制剂，并证明siRNA敲低的实用性。第二个目标将测试的假设，即蛋白激酶C是一个不可分割的一部分，在膀胱平滑肌收缩的调节信号和蛋白激酶C的特定亚型参与在这个信号的特定步骤。我们还将检验蛋白激酶C影响Rho激酶活性的假设。第三个目的是研究Rho激酶在膀胱平滑肌收缩调节中的作用。我们将测试的假设，一个组成性的活性，拉伸依赖性Rho激酶设置膀胱平滑肌的基础张力和第二个Rho激酶参与调节MLC磷酸酶活性。这些研究将使我们能够开发一个详细的，膀胱平滑肌调节的机制模型，我们将使用该模型来构建旨在了解在BPH等疾病状态下发生的调节变化的研究。 公共卫生相关性：该提案旨在了解膀胱平滑肌的功能。有几种膀胱疾病会显著影响生活质量。不幸的是，我们对正常膀胱的调节知之甚少，这是很难研究病变膀胱。本申请中提出的研究将提供这些缺失的信息。如果我们能了解正常膀胱是如何被控制的，我们就可以设计实验来研究并有望修复异常膀胱。