Regulation of Calcium Signaling in Retinal Ganglion Cells after Nerve Injury
神经损伤后视网膜神经节细胞钙信号传导的调节
基本信息
- 批准号:7930758
- 负责人:
- 金额:--
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2011
- 资助国家:美国
- 起止时间:2011-07-01 至 2015-06-30
- 项目状态:已结题
- 来源:
- 关键词:AffectApoptosisAxonAxotomyBlast InjuriesBlindnessBlunt TraumaCalcium SignalingCell DeathCell SurvivalCellsCharacteristicsClinicalComplexCraniocerebral TraumaDevelopmentDiseaseElectrophysiology (science)EyeEye InjuriesEye diseasesFaceFree RadicalsFrequenciesFunctional disorderGeneral PopulationGenesGlaucomaGliosisGoalsHeadHealthHealthcareHourImageImmuneImmunohistochemistryInjuryInvestigationKnowledgeLeadLigationMediatingMembraneModelingMusNerveNerve CrushNeurotransmittersOptic NerveOptic Nerve InjuriesOptic Nerve TransectionsOpticsPhysiologicalProgram ReviewsPropertyProteinsRecoveryRegulationReportingRetinaRetinalRetinal Ganglion CellsRoleSignal TransductionSmall Interfering RNAStrokeStructureSwellingTestingTraumaTraumatic Brain InjuryUp-RegulationVascular DiseasesVeteransVisionVisualWestern Blottingcell injurychannel blockerschronic painganglion cellinjurednerve injurynovelnovel strategiesoptic nerve disorderpatch clampresearch studyresponsesciatic nervetooltreatment strategyvectorvoltage
项目摘要
DESCRIPTION (provided by applicant):
Ocular and traumatic brain injuries (TBI) from blunt trauma or blast injury to the head occur with high frequency on the battlefield, and they are often accompanied by multiple visual dysfunctions, acuity loss and blindness in one or both eyes. Optic neuropathies are characterized by primary injury to the optic nerve, and loss of ganglion cells and their axons. Ganglion cell death is mediated in part by excessive intracellular Ca2+ ([Ca2+]i) loads following injury. Consistent with this finding is the enhancement of retinal ganglion cell survival after optic nerve crush with the administration of Ca2+ channel antagonists, which inhibit both L- and T-type Ca2+ currents, and reduce secondary ganglion cell death. The rationale underlying the proposed studies is that reduction of ganglion cell intracellular Ca2+ levels by regulation of Ca2+ channel activity may be an important component of protective strategies for the treatment of retinal injury. Suppression of excessively elevated [Ca2+]i in ganglion cells would provide a temporal window for ganglion cell survival and axonal recovery following injury. Proposed studies will test the hypothesis that suppression of elevated [Ca2+]i following nerve injury enhances ganglion cell survival. Specific aim 1 will define the signaling role of L- and T-type Ca2+ channels, and their accessory proteins (23 and 124) in mouse retinal ganglion cells. Experiments will determine a) the expression of L- and T-type Ca2+ channels and their accessory proteins by ganglion cells, and b) characterize the physiological and biophysical properties of L- and T-type Ca2+ currents of ganglion cells. Specific aim 2 will test the hypothesis that ganglion cell Ca2+ signaling is dysregulated immediately following and several days after optic nerve crush or transection. Investigations will determine if there are short (12 and 24 hours)- and long (10 and 20 days)-term alterations of a) the expression of L- and T-type, and 23 and 124 Ca2+ channel subunits by ganglion cells, and b) membrane mechanisms that mediate Ca2+ currents and signaling in ganglion cells following optic nerve injury. Specific aim 3 will test the hypothesis that Ca2+ channel antagonists and small interfering RNA (siRNA) antisense Ca2+ channel subunit vectors regulate Ca2+ signaling, and enhance ganglion cell survival after optic nerve injury. Investigations will determine if a) the L- and T-type Ca2+ channel antagonist, lomerizine, and b) antisense T-type (CaV3.1 and CaV3.2), and 23 and 124 Ca2+ channel subunit siRNA vectors, modulate Ca2+ signaling and enhance ganglion cell survival following optic nerve injury. Proposed studies will elucidate Ca2+ signaling in normal and injured ganglion cells, and develop novel approaches for controlling elevated intracellular Ca2+ following nerve injury, which will enhance ganglion cell survival, a key step in saving vision. These studies are consistent with the health-related goals of the Veterans Adminstration to develop highly effective and novel treatments for eye injury and disease.
PUBLIC HEALTH RELEVANCE:
Project Narrative Traumatic brain injury (TBI) is a common casualty in the battlefield. Ocular trauma frequently occurs with TBI, which results in visual impairments, including acuity loss and blindness often due to optic nerve and retina injury. This Merit Review application will test the hypothesis that suppression of elevated intracellular Ca2+ induced by nerve injury enhances ganglion cell survival, a key step in saving vision. Planned studies will use animal models of ocular nerve injury and test novel strategies for controlling Ca2+ signaling using Ca2+ channel antagonists and antisense siRNAs for Ca2+ channels to reduce ganglion cell loss, thus setting the stage for developing new therapeutic approaches to ameliorate ocular damage and vision. These investigations are consistent with the health-related goals of the Department of Veteran Affairs to develop highly effective treatments for eye injuries and disease, and to prevent impaired vision and blindness.
描述(由申请人提供):
战场上头部钝器伤或爆炸伤造成的眼部和创伤性脑损伤(TBI)发生率很高,通常伴有一只或两只眼睛的多种视觉功能障碍、视力丧失和失明。视神经病变的特征在于视神经的原发性损伤以及神经节细胞及其轴突的损失。神经节细胞死亡部分由损伤后过量的细胞内Ca 2+([Ca 2 +]i)负荷介导。与这一发现相一致的是,在视神经挤压后,施用Ca 2+通道拮抗剂可增强视网膜神经节细胞的存活,其抑制L型和T型Ca 2+电流,并减少继发性神经节细胞死亡。提出的研究的基本原理是,通过调节Ca 2+通道活性来降低神经节细胞内Ca 2+水平可能是治疗视网膜损伤的保护策略的重要组成部分。抑制神经节细胞中过度升高的[Ca 2 +]i将为损伤后神经节细胞存活和轴突恢复提供时间窗。拟开展的研究将检验神经损伤后抑制[Ca 2 +]i升高可增强神经节细胞存活的假设。具体目标1将定义L型和T型Ca 2+通道及其辅助蛋白(23和124)在小鼠视网膜神经节细胞中的信号传导作用。实验将确定a)L-和T-型Ca 2+通道及其辅助蛋白在神经节细胞中的表达,和B)表征神经节细胞的L-和T-型Ca 2+电流的生理和生物物理特性。具体目标2将检验神经节细胞Ca 2+信号传导在视神经挤压或横断后立即和几天后失调的假设。研究将确定视神经损伤后,a)L型和T型以及23和124 Ca 2+通道亚单位的表达,和B)介导Ca 2+电流和神经节细胞信号传导的膜机制是否存在短期(12和24小时)和长期(10和20天)变化。具体目标3将检验Ca 2+通道拮抗剂和小干扰RNA(siRNA)反义Ca 2+通道亚基载体调节Ca 2+信号传导并增强视神经损伤后神经节细胞存活的假设。研究将确定a)L型和T型Ca 2+通道拮抗剂洛美利嗪和B)反义T型(CaV3.1和CaV3.2)以及23和124 Ca 2+通道亚基siRNA载体是否调节视神经损伤后的Ca 2+信号传导并增强神经节细胞存活。拟议的研究将阐明正常和受伤的神经节细胞中的Ca 2+信号传导,并开发新的方法来控制神经损伤后细胞内Ca 2+的升高,这将提高神经节细胞的存活率,这是挽救视力的关键一步。这些研究与退伍军人管理局的健康相关目标是一致的,即为眼损伤和疾病开发高效和新颖的治疗方法。
公共卫生关系:
创伤性脑损伤(TBI)是战场上常见的伤亡。眼外伤经常与TBI一起发生,其导致视觉障碍,包括通常由于视神经和视网膜损伤而导致的敏锐度丧失和失明。此Merit Review应用程序将测试抑制神经损伤诱导的细胞内Ca 2+升高可增强神经节细胞存活的假设,这是挽救视力的关键步骤。计划中的研究将使用眼神经损伤的动物模型,并测试使用Ca 2+通道拮抗剂和Ca 2+通道的反义siRNA控制Ca 2+信号传导的新策略,以减少神经节细胞损失,从而为开发新的治疗方法以改善眼损伤和视力奠定基础。这些研究与退伍军人事务部的健康相关目标一致,即开发高效的眼损伤和疾病治疗方法,并预防视力受损和失明。
项目成果
期刊论文数量(0)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
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NICHOLAS C. BRECHA其他文献
NICHOLAS C. BRECHA的其他文献
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{{ truncateString('NICHOLAS C. BRECHA', 18)}}的其他基金
VRC: Reduction of Vision Loss with Early Interventions After Optic Nerve Injury
VRC:视神经损伤后早期干预可减少视力丧失
- 批准号:
10597946 - 财政年份:2022
- 资助金额:
-- - 项目类别:
Horizontal cell signaling in the mammalian retina
哺乳动物视网膜中的水平细胞信号传导
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10090603 - 财政年份:2019
- 资助金额:
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Horizontal cell signaling in the mammalian retina
哺乳动物视网膜中的水平细胞信号传导
- 批准号:
10331735 - 财政年份:2019
- 资助金额:
-- - 项目类别:
Horizontal cell signaling in the mammalian retina
哺乳动物视网膜中的水平细胞信号传导
- 批准号:
10547806 - 财政年份:2019
- 资助金额:
-- - 项目类别:
Regulation of Calcium Signaling in Retinal Ganglion Cells after Nerve Injury
神经损伤后视网膜神经节细胞钙信号传导的调节
- 批准号:
8278451 - 财政年份:2011
- 资助金额:
-- - 项目类别:
Regulation of Calcium Signaling in Retinal Ganglion Cells after Nerve Injury
神经损伤后视网膜神经节细胞钙信号传导的调节
- 批准号:
8397567 - 财政年份:2011
- 资助金额:
-- - 项目类别:
Regulation of Calcium Signaling in Retinal Ganglion Cells after Nerve Injury
神经损伤后视网膜神经节细胞钙信号传导的调节
- 批准号:
8696777 - 财政年份:2011
- 资助金额:
-- - 项目类别:
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