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首页> 外文期刊>Journal of stem cells. >Biomarker discovery and biotherapeutics applications of photosynthetic light-harvesting and bioluminescence light-emitting chromophore-protein complexes in stem cell biology and regenerative medicine.
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Biomarker discovery and biotherapeutics applications of photosynthetic light-harvesting and bioluminescence light-emitting chromophore-protein complexes in stem cell biology and regenerative medicine.

机译:干细胞生物学和再生医学中光合光捕获和生物发光发色团蛋白复合物的生物标志物发现和生物治疗学应用。

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摘要

We have since the 1970's embarked on the development of biologically derived fluorophore-protein complexes that will find applications in the communicable and non-communicable disease etiology processes and their cures. We have since then become largely successful in these endeavors along with interspersed contributions also from investigators who have generally restricted to working in confined disciplines. Their encompassment with our works as this investigator has traversed his definitely chosen and not merely a circumstantial, coincidental, or accidental step-wise multi-disciplinary scientific path from biophysics to regenerative medicine spanning these lines of investigations for last four decades have finally yielded the much necessitated disease related applied biological interventions for human benefits. Taking a cue from our early investigations and findings on which we call attention to the identification and characterization of the use of the primary light-emitting lumazine precursor of riboflavin which is 6,7-dimethyl-8-ribityl lumazine-protein complex which we had derived from the bioluminescence bacterium (Photobacterium phosphoreum) wherein it functions as a naturally occurring fluorescence light emitter (LumP). These in vivo phenomena have been a precursor to the subsequent developments in vitro. This in vivo to in vitro investigation path of ours has been also comprised among others of binding of photosynthetic light-harvesting marine dinoflagellate algae (Glenodinium sp.) derived peridinin-chlorophyll a-protein (PerCP) complex-labeled monoclonal antibodies useful in the development of flow cytometry. These fluorescence labeled antibodies bound antigens which include those of communicable infectious diseases (HIV/AIDS - env-gp160, gag-p24), non-communicable but also potential hereditary and malignant disorders (Cancer/Tumor Markers - Melan-A/Mart-1 of melanoma), normal immune response cells (Human/Mouse/species cellular MHC/TCR/CD45/CD33/CD56/CD19/CD41), and of types of stem cells (CD34/CD38/c-Mpl/Oct4/Neuropilin-1/SOX17). Such antigens have been analyzed by us and other investigators by fluorescence-activated cell sorting (FACS - cell surface and intracellular binding), confocal fluorescence microscopy, or/and immunohistochemistry, to determine qualitative and quantitative antigen expression levels and their mechanistic implications. We have followed stem cell differentiation patterns and signaling mechanisms through marker antigen-antibody binding wherein the antibodies are labeled with covalently linked fluorophore-protein complexes or fluorescence emitting chromophores. These complexes among others also have included PerCP. We are also now in the process of developing flow cytometry applications of additional visible light emitting chromophore-protein complexes through industrial collaborations. The United States Navy has long been known for interest in the estimation of changes in illumination intensity in and under the oceans to track movements of enemy ships and other naval vessels.
机译:自1970年代以来,我们就着手开发生物衍生的荧光团-蛋白质复合物,该复合物将在传染性和非传染性疾病的病因学过程及其治疗中得到应用。从那时起,我们在这些工作中取得了很大的成功,同时调查人员的穿插贡献也大为成功,他们通常只限于在受限领域工作。在过去的几十年中,作为该研究人员的研究对象,他们遍历了他的绝对选择,而不仅仅是从生物学到再生医学的偶然,偶然或偶然的逐步多学科科学路径,跨越了这些研究领域,最终产生了很多必需的疾病相关的应用生物干预措施才能造福人类。从我们的早期研究和发现中汲取线索,在这些研究和发现中,我们提请注意核黄素的主要发光lumazine前体的使用和鉴定,该前体是我们拥有的6,7-二甲基-8-ribityl lumazine-蛋白质复合物。衍生自生物发光细菌(Photobacteriumphosphorum),其中它起天然荧光发射体(LumP)的作用。这些体内现象是体外后续发展的先驱。我们的这种从体内到体外的研究路径还包括与光合作用的光捕获海洋鞭毛藻藻(Glenodinium sp。)衍生的苦瓜素-叶绿素a蛋白(PerCP)复合物标记的单克隆抗体的结合,这些抗体可用于开发流式细胞仪。这些荧光标记的抗体结合的抗原包括传染性传染病(HIV / AIDS-env-gp160,gag-p24),非传染性以及潜在的遗传和恶性疾病的抗原(癌症/肿瘤标志物-Melan-A / Mart-1黑色素瘤),正常免疫反应细胞(人类/小鼠/物种MHC / TCR / CD45 / CD33 / CD56 / CD19 / CD41)和干细胞类型(CD34 / CD38 / c-Mpl / Oct4 / Neuropilin-1) / SOX17)。我们和其他研究人员已经通过荧光激活细胞分选(FACS-细胞表面和细胞内结合),共聚焦荧光显微镜或/和免疫组织化学法对此类抗原进行了分析,以确定定性和定量的抗原表达水平及其机理。通过标记物抗原-抗体结合,我们遵循了干细胞分化模式和信号传导机制,其中抗体被共价连接的荧光团-蛋白质复合物或发射荧光的生色团标记。这些复合体还包括PerCP。我们现在也正在通过工业合作开发其他可见光发色团-蛋白质复合物的流式细胞术应用。长期以来,美国海军一直对估计海洋中和水下的光照强度变化以跟踪敌舰和其他海军舰船的运动感兴趣。

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  • 来源
    《Journal of stem cells.》 |2014年第3期|共7页
  • 作者

    KokaP.S.;

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  • 正文语种 eng
  • 中图分类 Q28;
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