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流式细胞术在HIV感染和艾滋病中的应用最新进展。

An update on the use of flow cytometry in HIV infection and AIDS.

作者信息

Hengel R L, Nicholson J K

机构信息

Division of Infectious Diseases, Department of Medicine, Georgetown University, Washington, DC, USA.

出版信息

Clin Lab Med. 2001 Dec;21(4):841-56.

Abstract

Flow cytometry has played an invaluable role in recent advances made against HIV and AIDS, and there is every reason to expect it will continue to do so. Newer-generation machines, using three- and four-color panels, make measurements of lymphocyte subsets ever more accurate and potentially cost-effective. Similarly, recent single-platform techniques promise even more efficiencies, freeing CD4 enumeration from parallel determination of the CBC. In other developments, quantitative reporting of immunophenotype may well change the way subsets traditionally defined by qualitative determinations are viewed. The most promising initial candidates for such changes are surrogates of immune activation, such as CD38 expression on CD8 cells. But technical demonstration of reproducibility and reliability, and clinical trial evidence of utility--especially as measured against such established laboratory parameters as CD4 cell and HIV RNA determinations--are needed before a change from qualitative to quantitative immunophenotype measurement can be widely accepted. Although too soon to tell if they will emerge from the research arena into the clinical arena, tetramer binding, intracellular cytokine detection, and assays of cell division are rapidly advancing understanding of HIV-disease, and indeed understanding of all of human immunology. Some of these assays provide often subtly different information, and together they will help determine the most important surrogate measures of clinical immunity. Identifying such surrogates is critical to developing a rational HIV vaccine. The power of flow cytometry is its ability simultaneously to analyze data in four, five, six, or more dimensions. For longitudinal experiments, time adds yet another dimension. Humans struggle to think past three dimensions; interpreting results from experimental permutations and combinations that expand geometrically with each additional parameter studied requires considerable effort. Ultimately computer programs might come to our aid, but for now we have to live with the information overload if we hope to gain insight into the workings of complex biologic systems. In a world of limited resources, and with limited capacity to conceptualize in multiple dimensions, insight, inspiration, and perhaps a little luck are needed to ask the right questions and use the right assays if the recent string of advances against AIDS is to continue.

摘要

流式细胞术在近年来抗击艾滋病毒和艾滋病的进展中发挥了极其重要的作用,而且完全有理由预计它将继续发挥这样的作用。新一代仪器采用三色和四色检测板,使淋巴细胞亚群的测量更加准确,且可能具有成本效益。同样,最近的单平台技术有望实现更高的效率,使CD4计数无需同时进行全血细胞计数。在其他进展方面,免疫表型的定量报告很可能会改变传统上通过定性测定定义的亚群的看待方式。这种变化最有希望的首批候选指标是免疫激活的替代指标,如CD8细胞上的CD38表达。但是,在从定性免疫表型测量转变为定量测量被广泛接受之前,需要有可重复性和可靠性的技术证明以及效用的临床试验证据——尤其是与CD4细胞和HIV RNA测定等既定实验室参数进行比较时。虽然现在还太早说它们是否会从研究领域进入临床领域,但四聚体结合、细胞内细胞因子检测和细胞分裂检测正在迅速推进对艾滋病毒疾病的理解,实际上也推进了对所有人免疫学的理解。其中一些检测提供的信息往往略有不同,它们将共同帮助确定临床免疫最重要的替代指标。确定这些替代指标对于开发合理的艾滋病毒疫苗至关重要。流式细胞术的强大之处在于它能够同时在四个、五个、六个或更多维度上分析数据。对于纵向实验,时间又增加了一个维度。人类很难超越三维去思考;解释随着研究的每个额外参数呈几何级数扩展的实验排列和组合的结果需要相当大的努力。最终计算机程序可能会帮助我们,但目前如果我们希望深入了解复杂生物系统的运作,就必须忍受信息过载。在资源有限且多维概念化能力有限的世界里,如果要延续最近一系列抗击艾滋病的进展,就需要洞察力、灵感,或许还需要一点运气来提出正确的问题并使用正确的检测方法。

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