Identification of gentamicin-binding proteins in the inner ear

内耳庆大霉素结合蛋白的鉴定

• 批准号: 7895731
• 负责人: Takatoshi Karasawa
• 金额: $ 15.25万
• 依托单位: OREGON HEALTH & SCIENCE UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2008
• 资助国家: 美国
• 起止时间: 2008-08-15 至 2012-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7895731
• 关键词: Acute Kidney Failure; Affect; Aminoglycoside Antibiotics; Aminoglycosides; Antibodies; Attenuated; Auditory; Bacterial Infections; Binding; Binding Proteins; Biochemical; Biological Assay; Cattle; Cell Death; Cell Line; Cells; Chemistry; Chronic; Confocal Microscopy; Coomassie blue; Cytoskeleton; Distal; Escherichia coli; Family suidae; Future; Gene Expression; Gentamicins; Goals; Hair Cells; Immunohistochemistry; In Vitro; Individual; Infant; Kidney; Labyrinth; Lead; Life; Mammalian Cell; Mass Spectrum Analysis; Microsomes; Molecular Chaperones; Nephrotoxic; Organ of Corti; Pathogenesis; Patients; Pattern; Pharmaceutical Preparations; Physiological; Play; Predisposition; Premature Infant; Prevention; Prophylactic treatment; Proteins; Proximal Kidney Tubules; Recombinant Proteins; Relative (related person); Reporting; Research; Risk; Role; Sensory Hair; Sepharose; Sodium Dodecyl Sulfate-PAGE; Staining method; Stains; Techniques; Tissues; Toxic effect; Wounds and Injuries; aminoglycoside-induced ototoxicity; calreticulin; cell type; cytotoxicity; deafness; equilibration disorder; immunocytochemistry; in vivo; insight; nephrotoxicity; novel; ototoxicity; prevent; protein E; protein expression; protein function

DESCRIPTION (provided by applicant): Aminoglycoside antibiotics like gentamicin are essential for battling life-threatening bacterial infections. Aminoglycosides also cause permanent deafness/balance disorders and nephrotoxicity in more than 120,000 individuals each year in the US, particularly in infants and premature babies. The long-term goal of this research is to prevent aminoglycoside-induced ototoxicity by modulating the functions of gentamicin-binding proteins crucial for ototoxicity, to preserve auditory function. In this proposal, we seek to identify gentamicin-binding proteins, and determine their distribution in the inner ear. We hypothesize that there are gentamicin-binding proteins in the inner ear, and that these proteins retain gentamicin in specific types of cells, contributing to cytotoxicity in vitro and pathogenesis in vivo. The specific aims of this project are: First, to identify gentamicin-binding proteins specific in kidney proximal tubule and cochlear cells. We will use a gentamicin-agarose pull-down assay and SDS-polyacrylamide gel electrophoresis to isolate such proteins from kidney proximal tubule and cochlear cell lines, and determine their identity using mass spectrometry (Aim 1). Second, to determine the distribution of gentamicin-binding proteins, including HSP73 and calreticulin, in the inner ear by immunocytochemistry and confocal microscopy. We will also determine if these proteins are co-localized with systemically-administered gentamicin, using fluorescently-tagged gentamicin or untagged gentamicin localized by gentamicin immunocytochemistry (Aim 2). If we can identify gentamicin-binding proteins that sequester the drug within cells that then induce cytotoxicity, we can develop new strategies to inhibit their interactions, and attenuate drug retention. Alternatively, if gentamicin-binding inhibits the functions of these proteins, we could use pharmacological activators of these proteins to overcome gentamicin-induced inhibition. Future studies will determine if gentamicin inhibits their interactions with physiological binding molecules/proteins, and if expression levels of gentamicin-binding proteins change during sustained treatment with gentamicin. Identification of gentamicin-binding proteins and their intracellular mechanisms that gentamicin interferes with to initiate cell death will provide new insight for clinicians to screen patients for pre-existing conditions and medications that elevate the risk of aminoglycoside toxicity and deafness. Identification of gentamicin-binding proteins that play a major role in gentamicin- induced ototoxicity is crucial in understanding how gentamicin induces ototoxicity and deafness. The proposed research will enable us to develop strategies to prevent interactions between gentamicin and gentamicin-binding proteins, and to overcome gentamicin-induced inhibition by pharmacologically activating the proteins. These strategies will lead to ototoxicity and deafness prevention.

描述（由申请人提供）：氨基糖苷类抗生素如庆大霉素对于对抗危及生命的细菌感染至关重要。在美国，氨基糖苷类药物每年也会导致超过120，000例永久性耳聋/平衡障碍和肾毒性，尤其是在婴儿和早产儿中。本研究的长期目标是通过调节对耳毒性至关重要的庆大霉素结合蛋白的功能来预防氨基糖苷类药物诱导的耳毒性，以保护听觉功能。在这个建议中，我们试图确定庆大霉素结合蛋白，并确定它们在内耳中的分布。我们假设内耳中存在庆大霉素结合蛋白，并且这些蛋白将庆大霉素保留在特定类型的细胞中，从而导致体外细胞毒性和体内发病机制。本课题的具体目标是：首先，鉴定肾近端小管和耳蜗细胞中庆大霉素特异性结合蛋白。我们将使用庆大霉素-琼脂糖下拉试验和SDS-聚丙烯酰胺凝胶电泳从肾近端小管和耳蜗细胞系中分离此类蛋白质，并使用质谱法确定它们的身份（目的1）。第二，通过免疫细胞化学和共聚焦显微镜确定庆大霉素结合蛋白（包括HSP 73和钙网蛋白）在内耳中的分布。我们还将确定这些蛋白质是否与全身给予的庆大霉素共定位，使用荧光标记的庆大霉素或通过庆大霉素免疫细胞化学定位的未标记的庆大霉素（目的2）。如果我们能够鉴定出庆大霉素结合蛋白，这些蛋白将药物隔离在细胞内，然后诱导细胞毒性，我们就可以开发新的策略来抑制它们的相互作用，并减弱药物滞留。或者，如果庆大霉素结合抑制这些蛋白质的功能，我们可以使用这些蛋白质的药理学激活剂来克服庆大霉素诱导的抑制。未来的研究将确定庆大霉素是否抑制它们与生理结合分子/蛋白的相互作用，以及庆大霉素结合蛋白的表达水平是否在庆大霉素持续治疗期间发生变化。确定庆大霉素结合蛋白及其细胞内机制，庆大霉素干扰启动细胞死亡，将为临床医生提供新的见解，以筛选患者的既存条件和药物，提高氨基糖苷类毒性和耳聋的风险。确定在庆大霉素诱导的耳毒性中起主要作用的庆大霉素结合蛋白对于理解庆大霉素如何诱导耳毒性和耳聋至关重要。拟议的研究将使我们能够开发策略，以防止庆大霉素和庆大霉素结合蛋白之间的相互作用，并克服庆大霉素诱导的抑制，通过抑制激活的蛋白质。这些策略将导致耳毒性和耳聋预防。

项目成果

Expression of proinflammatory and proangiogenic cytokines in patients with head and neck cancer.

• 发表时间: 1999-06
• 期刊: Clinical cancer research : an official journal of the American Association for Cancer Research
• 作者: Zhong Chen;Pramit S. Malhotra;G. Thomas;F. Ondrey;D. Duffey;Conrad W. Smith;Ileana I. Enamorado

Effects of the novel alphav integrin antagonist SM256 and cis-platinum on growth of murine squamous cell carcinoma PAM LY8.

新型αv整合素拮抗剂SM256和顺铂对小鼠鳞状细胞癌PAM LY8生长的影响。

• DOI: 10.3892/ijo.16.6.1189
• 发表时间: 2000
• 期刊: International journal of oncology
• 影响因子: 5.2
• 作者: VanWaes,C;Enamorado-Ayala,I;Hecht,D;Sulica,L;Chen,Z;Batt,DG;Mousa,S
• 通讯作者: Mousa,S