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Edward B. Ziff

Researcher at New York University

Publications -  136
Citations -  18236

Edward B. Ziff is an academic researcher from New York University. The author has contributed to research in topics: AMPA receptor & PDZ domain. The author has an hindex of 60, co-authored 134 publications receiving 17745 citations. Previous affiliations of Edward B. Ziff include Howard Hughes Medical Institute.

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Structure of the gene encoding peripherin, an NGF-regulated neuronal-specific type III intermediate filament protein.

TL;DR: Cloned rat gene encoding peripherin demonstrates that peripherin is a type III intermediate filament protein that is NGF-regulated, and the peripherin promoter contains sequences homologous to regions of other N GF-regulated promoters, which may function in peripherin induction by NGF.
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Bidirectional regulation of neuronal nitric-oxide synthase phosphorylation at serine 847 by the N-methyl-D-aspartate receptor.

TL;DR: The reversibility of NMDA receptor-induced phosphorylation at Ser847 by different doses of glutamate suggests two mechanisms with opposite effects: a time-dependent negative feedback induced by physiological concentrations of glutamate that limits nNOS activation and precludes the overproduction of NO; and a pathological stimulation by high concentrations of glutamatergic glutamate that leads to unregulated nN OS activation and production of toxic levels of NO.
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TARPs and the AMPA Receptor Trafficking Paradox

TL;DR: This review considers how transmembrane AMPAR regulatory proteins (TARPs), a novel family of AMPAR auxiliary subunits, have changed the authors' view of AM PAR transport and raised some perplexing questions.
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Transactivation of c-fos and β-actin genes by raf as a step in early response to transmembrane signals

TL;DR: These findings indicate that raf kinase, when activated by a transmembrane signal or by mutation of a regulatory domain, can phosphorylate a factor(s) capable of regulating transcription of the c-fos and actin genes.
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Differential palmitoylation directs the AMPA receptor-binding protein ABP to spines or to intracellular clusters.

TL;DR: A variant of ABP-L is reported that is palmitoylated at a cysteine residue at position 11 within a novel 18 amino acid N-terminal leader sequence encoded through differential splicing, indicating that targeting the protein to spines is dependent onPalmitoylation.