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Adam J. Bogdanove

Researcher at Cornell University

Publications -  116
Citations -  16667

Adam J. Bogdanove is an academic researcher from Cornell University. The author has contributed to research in topics: TAL effector & Effector. The author has an hindex of 43, co-authored 111 publications receiving 15043 citations. Previous affiliations of Adam J. Bogdanove include University of Minnesota & BASF SE.

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Efficient design and assembly of custom TALEN and other TAL effector-based constructs for DNA targeting

TL;DR: A method and reagents for efficiently assembling TALEN constructs with custom repeat arrays are presented and design guidelines based on naturally occurring TAL effectors and their binding sites are described.
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A Simple Cipher Governs DNA Recognition by TAL Effectors

TL;DR: It is shown that a repeat-variable pair of residues specifies the nucleotides in the target site, one pair to one nucleotide, with no apparent context dependence, which represents a previously unknown mechanism for protein-DNA recognition that explains TAL effector specificity, enables target site prediction, and opens prospects for use of TAL effects in research and biotechnology.
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Targeting DNA Double-Strand Breaks with TAL Effector Nucleases

TL;DR: A new class of sequence-specific nucleases created by fusing transcription activator-like effectors (TALEs) to the catalytic domain of the FokI endonuclease is reported.
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TAL effectors: Customizable proteins for DNA targeting

TL;DR: Comprising tandem, polymorphic amino acid repeats that individually specify contiguous nucleotides in DNA, this domain is being deployed in DNA targeting for applications ranging from understanding gene function in model organisms to improving traits in crop plants to treating genetic disorders in people.
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Understanding the functions of plant disease resistance proteins.

TL;DR: Many disease resistance (R) proteins of plants detect the presence of disease-causing bacteria, viruses, or fungi by recognizing specific pathogen effector molecules that are produced during the infection process.