Publications by authors named "Shahar Amitai"

Solid-oxide fuel cells produce electric current from energy released by a spontaneous electrochemical reaction. The efficiency of these devices depends crucially on the microstructure of their electrodes and in particular on the three-phase boundary (TPB) length, along which the energy-producing reaction occurs. We present a systematic maximization of the TPB length as a function of four readily controllable microstructural parameters, for any given mean hydraulic radius, which is a conventional measure of the permeability to gas flow.

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We identify two orthogonal sources of structural entropy in rattler-free granular systems: affine, involving structural changes that only deform the contact network, and topological, corresponding to different topologies of the contact network. We show that a recently developed connectivity-based granular statistical mechanics separates the two naturally by identifying the structural degrees of freedom with spanning trees on the graph of the contact network. We extend the connectivity-based formalism to include constraints on, and correlations between, degrees of freedom as interactions between branches of the spanning tree.

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We first show that the currently accepted statistical mechanics for granular matter is flawed. The reason is that it is based on the volume function, which depends only on a minute fraction of all the structural degrees of freedom and is unaffected by most of the configurational microstates. Consequently, the commonly used partition function underestimates the entropy severely.

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Escherichia coli (E. coli) mazEF is a stress-induced toxin-antitoxin (TA) module. The toxin MazF is an endoribonuclease that cleaves single-stranded mRNAs at ACA sequences.

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The Escherichia coli mazEF module is one of the most thoroughly studied toxin-antitoxin systems. mazF encodes a stable toxin, MazF, and mazE encodes a labile antitoxin, MazE, which prevents the lethal effect of MazF. MazF is an endoribonuclease that leads to the inhibition of protein synthesis by cleaving mRNAs at ACA sequences.

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Traditionally, programmed cell death (PCD) is associated with eukaryotic multicellular organisms. However, recently, PCD systems have also been observed in bacteria. Here we review recent research on two kinds of genetic programs that promote bacterial cell death.

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mazEF is a toxin-antitoxin module located on the Escherichia coli chromosome and that of some other bacteria, including pathogens. mazF specifies for a stable toxin, MazF, and mazE specifies for a labile antitoxin, MazE, that antagonizes MazF. MazF is a sequence-specific mRNA endoribonuclease that initiates a programmed cell death pathway in response to various stresses.

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mazEF is a stress-induced toxin-antitoxin module, located on the chromosome of Escherichia coli, that we have previously described to be responsible for programmed cell death in E. coli. mazF specifies a stable toxin, and mazE specifies a labile antitoxin.

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