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Programmable Daisychaining of Microelectrodes for IP Protection in MEDA Biochips

机译:在Meda Biochips中的IP保护微电极的可编程DaiSCONALING

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As digital microfluidic biochips (DMFBs) make the transition to the marketplace for commercial exploitation, security and intellectual property (IP) protection are emerging as important design considerations. Recent studies have shown that DMFBs are vulnerable to reverse engineering aimed at stealing biomolecular protocols (IP theft). The IP piracy of proprietary protocols may lead to significant losses for pharmaceutical and biotech companies. The micro-electrode-dot-array (MEDA) is a next-generation DMFB platform that supports real-time sensing of droplets and has the added advantage of important security protections. However, real-time sensing offers opportunities to an attacker to steal the biochemical IP. We show that the daisychaining of microelectrodes and the use of one-time-programmability in MEDA biochips provides effective bitstream scrambling of biochemical protocols. To examine the strength of this solution, we develop a SAT attack that can unscramble the bitstreams through repeated observations of bioassays executed on the MEDA platform. Based on insights gained from the SAT attack, we propose an advanced defense against IP theft. Simulation results using real-life biomolecular protocols confirm that while the SAT attack is effective for simple instances, our advanced defense can thwart it for realistic MEDA biochips and real-life protocols.
机译:作为数字微流体Biochips(DMFBs)使向市场过渡到商业开发,安全和知识产权(IP)保护是出现的重要设计考虑因素。最近的研究表明,DMFBS容易受到旨在窃取生物分子协议(IP盗窃)的逆向工程。专有议定书的知识产权盗版可能导致制药和生物技术公司的重大损失。微电极 - 点阵列(MEDA)是一个下一代DMFB平台,支持液滴的实时感测,并具有重要的安全保护的额外优势。然而,实时感知为攻击者提供了窃取生物化学IP的机会。我们表明,在Meda Biochips中的微电极和使用一次性可编程性的DaiScoming提供了生化协议的有效比特流争先恐后的争先恐后的争先恐后的争先恐后。为了检查该解决方案的强度,我们开发了一种可以通过在Meda平台上执行的生物测定的反复观察来解读比特流的SAT攻击。根据SAT攻击所获得的洞察力,我们提出了对IP盗窃的先进防御。使用现实生物分子协议的仿真结果证实,虽然SAT攻击对于简单的实例有效,但我们的先进防御可以挫败它,以实现现实的地图生物芯片和现实生活协议。

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