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Lawrence D'Antonio

Researcher at Ramapo College

Publications -  18
Citations -  1010

Lawrence D'Antonio is an academic researcher from Ramapo College. The author has contributed to research in topics: Gene & Curriculum. The author has an hindex of 7, co-authored 18 publications receiving 852 citations.

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QGRS Mapper: a web-based server for predicting G-quadruplexes in nucleotide sequences

TL;DR: A web-based server that predicts quadruplex forming G-rich sequences (QGRS) in nucleotide sequences and features interactive graphic representation of the data is developed, very useful for investigating the functional relevance of G-quadruplex structure, in particular its role in regulating the gene expression by alternative processing.
Journal ArticleDOI

GRSDB2 and GRS_UTRdb: databases of quadruplex forming G-rich sequences in pre-mRNAs and mRNAs.

TL;DR: The goal of these experiments has been to build freely accessible resources for exploring the role of G-quadruplex structure in regulation of gene expression at post-transcriptional level.
Journal ArticleDOI

GRSDB: a database of quadruplex forming G-rich sequences in alternatively processed mammalian pre-mRNA sequences

TL;DR: The computational approach is applied to map putative Quadruplex forming GRSs within the transcribed regions of a large number of alternatively processed human and mouse gene sequences that were obtained as fully annotated entries from GenBank and RefSeq to build the GRSDB database, which provides a unique avenue for studying G-quadruplexes in the context of RNA processing sites.
Proceedings ArticleDOI

Computational methods for predicting intramolecular G-quadruplexes in nucleotide sequences

TL;DR: This suite of computational tools contains algorithms to search genes for occurrences of the G-quadruplex motif and determine their distribution near RNA processing sites.
Journal ArticleDOI

Role of conserved cis-regulatory elements in the post-transcriptional regulation of the human MECP2 gene involved in autism

TL;DR: The studies suggest that MECP2 post-transcriptional gene expression could be regulated by several evolutionarily conserved cis-elements like G-quadruplex motifs, microRNA target sites, and AU-rich elements.