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DNA sequence alignment: A review of hardware accelerators and a new core architecture

机译:DNA序列比对:硬件加速器和新核心架构的综述

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Deoxyribonucleic Acid (DNA) sequence alignment is essentially a way of comparing two or more DNA sequences with aim to find regions of similarities among them. The Smith-Waterman (SW) algorithm is a local alignment algorithm which is able to identify mutation in DNA sequences. However, the aforementioned algorithm tends to be slower in computation of long DNA sequences. Over decades ago, Field Programmable Gate Arrays (FPGAs) play an important role in DNA sequence alignment. Moreover, pipelining technique is also a well-known method used to speed-up the performance of hardware design. Systolic array (SA)-based DNA sequence alignment architecture reduces execution time of alignment matrix computation from quadratic to linear time complexity. In this paper, existing FPGA-based sequence alignment core architectures will be discussed followed by proposal for a new SA-based DNA sequence alignment core architecture. The design was synthesized on the Xilinx Spartan-3E XC3S1600E-FG3205. Results showed that the developed core architecture is 1.2× faster in speed as compared to other reported FPGA-based designs.
机译:脱氧核糖核酸(DNA)序列比对本质上是比较两个或多个DNA序列的一种方法,目的是在它们之间找到相似区域。 Smith-Waterman(SW)算法是一种局部比对算法,能够识别DNA序列中的突变。但是,上述算法在长DNA序列的计算中往往较慢。几十年前,现场可编程门阵列(FPGA)在DNA序列比对中起着重要作用。此外,流水线技术也是用于加速硬件设计性能的一种众所周知的方法。基于脉动阵列(SA)的DNA序列比对体系结构将比对矩阵计算的执行时间从二次到线性时间复杂度降低了。在本文中,将讨论现有的基于FPGA的序列比对核心架构,然后提出新的基于SA的DNA序列比对核心架构的建议。该设计在Xilinx Spartan-3E XC3S1600E-FG3205上进行了综合。结果表明,与其他已报告的基于FPGA的设计相比,已开发的内核架构的速度提高了1.2倍。

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