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Titlebook: Vascular Disease; Molecular Biology an Andrew H. Baker Book 1999 Humana Press 1999

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楼主: Callow
发表于 2025-3-26 22:48:56 | 显示全部楼层
Yutaka Kitami,Kunio Hiwada the system‘s viability kernel. We give results pertaining to certain continuity properties of the viability kernel, we give conditions under which the viability kernel can be computed in a finite number of steps, and we synthesize a hybrid controller that yields all viable trajectories.
发表于 2025-3-27 01:44:46 | 显示全部楼层
Rosalind P. Fabunmin in the first version of the mutual-exclusion protocol..We stress the fact that Fischer‘s protocol has been analyzed many times, using other real-time verification tools. in particular in [2, 13]. None of these two analyses, however, deals with starvation, while the versions of the protocol used ar
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Ulrich Laufs,James K. Liaoars at Lund. Leveraging these, we are led to our main contribution: a general set of hybrid systems model classes which encompass HDS and hence several other models popularized in the literature that combine finite automata and discrete event systems with ordinary differential (ODES) and differentia
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Todd Bourcierf real-time, distributed, and dynamic environment found in highly reconfigurable systems. Here, we discuss challenges, solutions, and lessons learned in the context of a long-term project at PARC to bring such techniques to a highly reconfigurable paper path system.
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and coordination..There are two broad classes of methods for dealing with these combined issues: one uses architectural means to separate them, so we can reason separately about hybrid control and fault tolerance, for example; the other integrates them, so that a single method is used to reason, for
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1543-1894 enetic influence. Part I describes three methods that have been used successfully to identify specific mutations in candidate genes involved in c- diovascular d978-1-61737-155-4978-1-59259-247-0Series ISSN 1543-1894 Series E-ISSN 1940-6037
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Radiation Hybrid (RH) Mapping of Human Smooth Muscle-Restricted Genes genes, including fluorescent in situ hybridization (FISH) (.) and interspecific mouse back-crossing (.). FISH analysis is relatively fast, but often requires large genomic clones and does not afford the high-resolution mapping required to link a gene locus to a disease phenotype. Interspecific mous
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