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ALCOHOLISM, GENES, AND HORMONES; TISSUE REPOSITORY

酗酒、基因和激素；

基本信息

批准号：
8174453
负责人：
Magdalena Uhart
金额：
$ 0.12万
依托单位：
LUNDQUIST INSTITUTE FOR BIOMEDICAL INNOVATION AT HARBOR-UCLA MEDICAL CENTER
依托单位国家：
美国
项目类别：
财政年份：
2009
资助国家：
美国
起止时间：
2009-12-01 至 2010-11-30
项目状态：
已结题

项目摘要

This subproject is one of many research subprojects utilizing the resources provided by a Center grant funded by NIH/NCRR. The subproject and investigator (PI) may have received primary funding from another NIH source, and thus could be represented in other CRISP entries. The institution listed is for the Center, which is not necessarily the institution for the investigator. In the study application, Pro00017519, we acknowledge that there may be analysis planned in the future regarding the data collected during this study. In addition, when the study was reviewed by the IRB, the Board strongly recommended that a separate IRB protocol be established to create a repository for future research. It was indicated that maximum benefit could be gained through the establishment of a separate repository protocol at CSMC for this study. Following the IRBs recommendation, we are proposing in our current application to establish a specimen/tissue and data repository. The current repository protocol will be established to collect, store and distribute specimens/tissue and/or data for future research. In the current protocol, the study team is proposing to: A. Collect blood sample that will be used to extract DNA from buffy coat isolation and/or lymphoblastoid cell lines to establish a repository at Cedars-Sinai Medical Center. The DNA collected for this repository study will provide an ongoing source of ¿normal¿ specimens to facilitate functional, molecular and genetic studies into the etiology of alcoholism and disease conditions in which the hormones and glands interact with the nervous system . This research may lead to new diagnostic, treatment and preventative strategies for alcoholism and neuroendocrine diseases. B. We are also proposing to collect blood samples during the daytime and nighttime alcohol sensitivity sessions described in protocol Pro00017519. The blood samples collected for this repository study will provide a source of specimens for future neuroendocrine measures. C. In addition, data collected at baseline and during the daytime and nighttime alcohol sensitivity sessions in protocol Pro00017519 will be used for future analysis determined by our research findings and those published in the literature. This repository will be established for the purpose of learning more about genetic and environmental risk factors for alcoholism and neuroendocrine disease conditions. The current repository protocol will be established to collect, store and distribute specimens and/or data for future research. In the current protocol, the study team is proposing to: A. Collect blood samples that will be used to extract DNA from buffy coat isolation and/or lymphoblastoid cell lines to establish a repository at Cedars-Sinai Medical Center. The DNA collected for this repository study will provide an ongoing source of ¿normal¿ specimens to facilitate functional, molecular and genetic studies into the etiology of alcoholism and neuroendocrine disease conditions. This research may lead to new diagnostic, treatment and preventative strategies for alcoholism and neuroendocrine diseases. B. We are also proposing to collect blood samples during the daytime and nighttime alcohol sensitivity sessions described in protocol Pro00017519. The blood samples collected for this repository study will provide a source of specimens for future neuroendocrine measures. C. In addition, data collected at baseline and during the daytime and nighttime alcohol sensitivity sessions in protocol Pro00017519 will be used for future analysis determined by our research findings and those published in the literature. The specimen/tissue sample collected for this repository study will provide an ongoing source of specimens to facilitate functional, molecular and genetic studies into the etiology of alcoholism and neuroendocrine disease conditions. This research may lead to new diagnostic, treatment and preventative strategies for alcoholism and neuroendocrine diseases. In addition, data collected will allow for future analysis determined by our research findings and those published in the literature.

该子项目是利用该技术的众多研究子项目之一资源由 NIH/NCRR 资助的中心拨款提供。子项目及研究者 (PI) 可能已从 NIH 的另一个来源获得主要资金，因此可以在其他 CRISP 条目中表示。列出的机构是对于中心来说，它不一定是研究者的机构。在研究申请 Pro00017519 中，我们承认未来可能计划对本研究期间收集的数据进行分析。此外，当 IRB 审查该研究时，委员会强烈建议建立单独的 IRB 协议，为未来的研究创建存储库。有人指出，通过在华润上华为本研究建立单独的存储库协议可以获得最大的利益。根据 IRB 的建议，我们建议在当前的申请中建立样本/组织和数据存储库。当前的存储库协议将被建立来收集、存储和分发样本/组织和/或数据以供未来研究。在当前的方案中，研究小组提议： A. 收集血样，用于从血沉棕黄层分离和/或类淋巴母细胞系中提取 DNA，以在 Cedars-Sinai 医疗中心建立储存库。为该储存库研究收集的DNA将提供持续的“正常”样本来源，以促进对酒精中毒和激素和腺体与神经系统相互作用的疾病的病因学的功能、分子和遗传学研究。这项研究可能会为酗酒和神经内分泌疾病带来新的诊断、治疗和预防策略。 B. 我们还建议在协议 Pro00017519 中描述的白天和夜间酒精敏感性会议期间收集血液样本。该储存库研究收集的血液样本将为未来的神经内分泌测量提供样本来源。 C. 此外，Pro00017519 方案中在基线以及白天和夜间酒精敏感性会议期间收集的数据将用于由我们的研究结果和文献中发表的结果确定的未来分析。建立该存储库的目的是为了更多地了解酗酒和神经内分泌疾病的遗传和环境风险因素。当前的存储库协议将被建立来收集、存储和分发样本和/或数据以供未来研究。在当前的方案中，研究小组提议： A. 收集血液样本，用于从血沉棕黄层分离和/或类淋巴母细胞系中提取 DNA，以在 Cedars-Sinai 医疗中心建立储存库。为该储存库研究收集的 DNA 将提供“正常”样本的持续来源，以促进对酗酒和神经内分泌疾病的病因学进行功能、分子和遗传学研究。这项研究可能会为酗酒和神经内分泌疾病带来新的诊断、治疗和预防策略。 B. 我们还建议在协议 Pro00017519 中描述的白天和夜间酒精敏感性会议期间收集血液样本。该储存库研究收集的血液样本将为未来的神经内分泌测量提供样本来源。 C. 此外，Pro00017519 方案中在基线以及白天和夜间酒精敏感性会议期间收集的数据将用于由我们的研究结果和文献中发表的结果确定的未来分析。为该储存库研究收集的标本/组织样本将提供持续的标本来源，以促进对酒精中毒和神经内分泌疾病的病因学的功能、分子和遗传学研究。这项研究可能会为酗酒和神经内分泌疾病带来新的诊断、治疗和预防策略。此外，收集的数据将允许根据我们的研究结果和文献中发表的结果进行未来的分析。