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Parallel simulation of apoptotic receptor-clustering on GPGPU many-core architectures

机译:GPGPU多核架构上凋亡受体簇的并行模拟

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Apoptosis, the programmed cell death, is a physiological process that handles the removal of unwanted or damaged cells in living organisms. The process itself is initiated by signaling through tumor necrosis factor (TNF) receptors and ligands, which form clusters on the cell membrane. The exact function of this process is not yet fully understood and currently subject of basic research. Different mathematical models have been developed to describe and simulate the apoptotic receptor-clustering. In this interdisciplinary work, a previously introduced model of the apoptotic receptor-clustering has been extended by a new receptor type to allow a more precise description and simulation of the signaling process. Due to the high computational requirements of the model, an efficient algorithmic mapping to a modern many-core GPGPU architecture has been developed. Such architectures enable high-performance computing (HPC) simulation tasks on the desktop at low costs. The developed mapping reduces average simulation times from months to days (peak speedup of 256x), allowing the productive use of the model in research.
机译:程序性细胞死亡是程序性细胞死亡,它是一种生理过程,负责处理生物体中不需要的或受损的细胞。该过程本身是通过在细胞膜上形成簇的肿瘤坏死因子(TNF)受体和配体发出信号而引发的。此过程的确切功能尚未完全了解,目前是基础研究的主题。已经开发了不同的数学模型来描述和模拟凋亡受体簇。在这项跨学科的工作中,以前引入的凋亡受体聚类模型已被新的受体类型扩展,从而可以更精确地描述和模拟信号传导过程。由于该模型的高计算要求,因此已经开发了到现代多核GPGPU架构的有效算法映射。这样的体系结构可以在桌面上以低成本实现高性能计算(HPC)仿真任务。开发的映射将平均模拟时间从数月缩短至数天(峰值加速为256倍),从而可以在研究中有效地使用模型。

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