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Algorithmic Challenges in Structural Molecular Biology and Proteomics

机译:结构分子生物学和蛋白质组学中的算法挑战

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This paper reviews our research in computational biology and chemistry. Some of the most challenging and influential opportunities for Physical Geometric Algorithms (PGA) arise in developing and applying information technology to understand the molecular machinery of the cell. Our recent work (e.g., [1-20]) shows that many PGA techniques may be fruitfully applied to the challenges of computational molecular biology. PGA research may lead to computer systems and algorithms that are useful in structural molecular biology, proteomics, and rational drug design. Concomitantly, a wealth of interesting computational problems arise in proposed methods for discovering new pharmaceuticals. I’ll briefly discuss some recent results from my lab, including new algorithms for interpreting X-ray crystallography [14, 17, 16] and NMR (nuclear magnetic resonance) data [3, 9, 6, 19, 10, 5, 7, 18, 4], disease classification using mass spectrometry of human serum [12], and protein redesign [13]. Our algorithms have recently been used, respectively, to reveal the enzymatic architecture of organisms high on the CDC bioterrorism watch-list [17, 16], for probabilistic cancer classification from human peripheral blood [12], and to redesign an antibioticproducing enzyme to bind a novel substrate [13]. I’ll overview these projects, and highlight some of the algorithmic and computational challenges.
机译:本文综述了我们在计算生物学和化学方面的研究。在开发和应用信息技术时出现了物理几何算法(PGA)的一些最具挑战性和有影响力的机会,以了解细胞的分子机械。我们最近的工作(例如,[1-20])表明,可以习惯于计算分子生物学的挑战来习惯效果效果效果。 PGA研究可能导致计算机系统和算法,可用于结构分子生物学,蛋白质组学和合理的药物设计。兼顾,有丰富的有趣的计算问题,以发现新药物的方法。我将简要讨论我实验室的一些最新结果,包括用于解释X射线晶体学的新算法[14,17,16]和NMR(核磁共振)数据[3,9,6,19,10,5,7 ,18,4],使用人血清质谱[12]和蛋白质重新设计[13]的疾病分类。最近,我们的算法分别用于揭示CDC生物恐怖主义观察列表[17,16]的生物体的酶促结构,用于从人周围血液[12]的概率癌症分类,并重新设计抗生素酶以结合一种新型底物[13]。我会概述这些项目,并突出一些算法和计算挑战。

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