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Toward noninvasive microspectrofluorometry of skin lesions for diagnostic and prognostic evaluation of cell metabolism and organelle interactions

机译:对皮肤病变的非侵入性微型分子荧光测定诊断和预后评估细胞代谢和细胞器相互作用的诊断和预后评价

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The basic principle of this approach relies on microspectrofluorometric observations of upheavals in the cell's energy metabolism and cell-to-cell metabolic communication in human and mouse melanoma cells. A striking feature is the definition of a highly active nuclear energy metabolism in M8255 human melanoma cells which is characterized by an intense fluorescence response associated with NAD(P) reduction by substrates of glycolysis or the hexose monophosphate shunt. Changes are also expected in the steady state levels of reduced/oxidized NAD(P) in the nuclear, cytoplasmic and mitochondrial compartments, which are probably dependent on ATP levels and distribution (as determined by cell metabolism and eventually the presence of ATP traps). A topographic scanning of skin lesions, either under metabolic steady state conditions or in the presence of permeating substrates, can lead to the recognition of characteristic patterns associated with pigmented and nonpigmented, malignant and nonmalignant skin lesions. The method is, in a way, an extension of microscopic transillumination techniques which have led to the identification of specific patterns associated with such lesions. However, here, a new dimension is added by introduction of fluorescence evaluations. This can represent the first step in a multiparameter approach to the non-invasive in situ fluorescence scan of dermatological lesions by inclusion of: (1) fluorescence excitation and emission spectra; (2) new fluorescence probes of cytoplasmic organelles and nuclear components. Primary emphasis should be placed on the highly active nuclear energy metabolism, which can be triggered to maximum levels when the role of mitochondria as the `cells's policeman' with regard to metabolic control is suppressed by use of topically cytotoxic agents such as the `antipsoriatic' anthralin and dicarboxylic acids used in the local treatment of melanoma. Fluorescence excitation spectroscopy may be of particular advantage in studies with the new highly sensitive cyanine nucleic acid dyes and their dimers, but caution should be exerted in the use of such compounds because of cytotoxicity (e.g., limiting it to cellular studies used in the interpretation of dermatological findings). Parallel cellular and non-invasive dermatological studies will help to define the most specific set of parameters to be used in diagnostic and prognostic evaluations of skin lesions.
机译:这种方法的基本原理依赖于在细胞的能量代谢和人和小鼠黑色素瘤细胞中的能量代谢和细胞对细胞代谢通信中的动力学分光荧光观察。引人注目的特征是M8255人黑素瘤细胞中具有高活性核能代谢的定义,其特征在于通过糖醇分解的果渣或己糖单磷酸酯分流的底物与NAD(P)还原相关的强烈的荧光反应。在核,细胞质和线粒体隔室中的稳态/氧化NAD(P)的稳态水平中也预期的变化可能取决于ATP水平和分布(如通过细胞代谢和最终存在ATP陷阱的存在)。皮肤病变的地形扫描,在代谢稳态条件下或在渗透基材的存在下,可以导致识别与着色和非染色的,恶性和非血管皮肤病变相关的特征模式。这种方法是一种方式,显微透射技术的延伸导致具有与这种病变相关的特定图案的识别。但是,这里,通过引入荧光评估来添加新的维度。这可以通过包含:(1)荧光激发和发射光谱来表示Mult-infaseRive的多次荧光扫描的多态荧光扫描的第一步。 (2)细胞质细胞器和核心组分的新荧光探针。初级重点应放在高度活跃的核能代谢上,当通过使用局部细胞毒性剂如“抗脂剂”等局部细胞毒性药物抑制了线粒体的作用,可以将线粒体的作用引发至最高水平。用于局部治疗黑色素瘤的蒽环和二羧酸。荧光激发光谱可能在使用新的高敏感的青色核酸染料及其二聚体的研究中特别有利,但是由于细胞毒性(例如,将其限制在解释中使用的细胞研究中,应施加这些化合物的谨慎皮肤病学发现)。平行细胞和非侵袭性皮肤病学研究将有助于定义用于在皮肤病变的诊断和预后评估中使用的最具体的参数。

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