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BIOGRAPHICAL SKETCH
NAME: Hoque, Mainul, Ph.D.
eRA COMMONS USER NAME (credential, e.g., agency login): hoquema
POSITION TITLE: Research Scientist
EDUCATION/TRAINING (Begin with baccalaureate or other initial professional education, such as
nursing, include postdoctoral training and residency training if applicable. Add/delete rows as
necessary.)
INSTITUTION AND LOCATION
DEGREE
(if applicable)
Completio
n Date
FIELD OF STUDY
MM/YYYY
University of Dhaka, Bangladesh
B.S
05/1990
Biochemistry
University of Dhaka, Bangladesh
M.Sc.
05/1992
Biochemistry
Tokyo Institute of Technology, Japan
Ph.D.
09/1999
Biotechnology
Rutgers Biomedical and Health Sciences
Postdoctoral
04/2004
Molecular virology
A. PERSONAL STATEMENT
I have been working in the field of molecular biology and genetics for more than fifteen years. I have
been studying various aspects of cellular and viral gene regulation using sate of the art molecular
biology tools throughout my research career. Since 2010 I have been working as a research scientist
at the New Jersey Medical School genomics research program where my primary role is to design,
execute and analysis of deep sequencing based experiments. Additionally, I have also been involved
in the development of sequencing based assays for both research and clinical genomics. I have
developed various techniques to study gene expression and RNA processing, including strandspecific RNA-seq, amplification-based 3’ end sequencing (3’-end-seq), and 3’ Region Extraction And
Deep Sequencing (3’READS). I also have substantial experience in ChIP-seq, CLIP-seq, and GROseq. I have been sequencing samples using Illumina HiSeq 2500, NextSeq500 and MiSeq platforms
to perform all our sequencing needs. I have been involved in designing and performing various deep
sequencing related experiment and maintaining the pipeline for the researchers of our school and
other collaborative institutes as demonstrated in the recent publications.
1. Dai W, Li W, Hoque M, Li Z, Tian B, and Makeyev E (2015). A post-transcriptional mechanism
pacing expression of neural genes with precursor cell differentiation status. Nature
communication. 6:7576. doi: 10.1038/ncomms8576.
2. Di Giammartino DC , Li W 2, Ogami K, Yashinskie JJ, Hoque M, Tian B, Manley JL. (2014).
RBBP6 isoforms regulate the human polyadenylation machinery and modulate expression of
mRNAs with AU-rich 3' UTRs. Genes Dev. 28(20):2248-60.
3. *Hoque M, *Ji Z, Zhang D, Luo W, Li W, Yehia G and Tian B. (2013). A method for mapping
3’end of transcripts and quantitative analysis of alternative polyadenylation isoform and gene
expression. Nat Methods 10(2): 133-139.
4. Luo W*, Ji Z*, Pan Z*, You B, Hoque M, Li W, Gunderson S. and Tian B. (2013). The conserved
intronic cleavage and polyadenylation site of CstF-77 gene imparts control of 3’ end processing by
feedback autoregulation and U1 snRNP. PLoS Genetics. 9, e1003613
B. POSITIONS AND HONORS
POSITIONS AND EMPLOYMENT
2000-2004 Postdoctoral Fellow, UMDNJ-New Jersey Medical School, Newark, NJ
2003-2007 Research Associate, UMDNJ-New Jersey Medical School, Newark, NJ
2007- 2013 Research Scientist, UMDNJ- New Jersey Medical School, Newark, NJ
2013- Present Adjunct Assistant Professor, Rutgers- New Jersey Medical School, Newark, NJ
AWARDS AND HONORS
1995
Japanese Government Scholarship, MONBUSHO
1999
Outstanding Research Scientist, Tokyo Institute of Technology
2009
Young Investigator Scholarship, Keystone Symposium
C. CONTRIBUTIONS IN SCIENCE
Since the beginning of my post-doctoral research I have been studying the role of cellular proteins in the
regulation of gene expression. I would like cite an example of a unique cellular protein called eIF5A. I have
shown that this very unique protein plays important role in the regulation of HIV gene expression, important
cancer genes as well nonsense mediated decay.
1. Mémin E, Hoque M, Jain MR, Heller DS, Li H, Cracchiolo BM, Hanauske HM, Pe’ery T and
Mathews MB*. (2014) Medicinal inhibition and silencing of eIF5A modification alter the expression
of malignancy-related genes and suppress cervical cancer cell proliferation. Cancer Research.
DOI: 10.1158/0008-5472
2. Hartmut M. HA*, Saxena D, Palumbo PE, Hanauske AR. Luchessi AD, Tavane D. Cambiaghi TD,
Hoque M, Spino M. , Gandolfi D, Heller DS, Singh S, Park MH, Cracchiolo BM, Tricta F, Connelly
J, Popowicz, AM, Cone1 RA, Holland B, Pe’ery T and Mathews, MB*. (2013). Drug-Induced
Reactivation of Apoptosis Abrogates HIV-1 Infection. PLOS ONE. 8(9): e74414.
doi:10.1371/journal.pone.0074414.
3. Hoque M, Hanauske-Abel HM, Palumbo P, Saxena D, D'Alliessi Gandolfi D, Park MH, Pe'ery T,
Mathews MB. (2009). Inhibition of HIV-1 replication by two drugs that prevent the maturation of
eIF5A. Retrovirology .6: 90-106.
I have studied the development of virus vector for ex vivo and in vivo gene therapy. My main focus
was to make changes in adeno-associated virus to develop a highly specific gene therapy vector,
which I believe is one of the most promising gene vector.
1. Hoque M, Ishizu K, Matsumoto A, Han SI, Arisaka F, Takayama M, Suzuki K, Kato K, Kanda T,
Watanabe H, Handa H. (1999). Nuclear transport of the major capsid protein is essential for
adeno-associated virus capsid formation. J Virol. 73:7912-7915.
2. Hoque M, Shimizu N, Ishizu K, Yajima H, Arisaka F, Suzuki K, Watanabe H, Handa H. (1999).
Chimeric virus-like particle formation of adeno-associated virus. Biochem Biophys Res Commun.
266: 371-376.
3. Ishizu KI, Watanabe H, Han SI, Kanesashi S N, Hoque M, Yajima H, Kataoka K, and Handa H.
(2001). Roles of disulfide linkage and calcium ion-mediated interactions in assembly and
disassembly of virus-like particles composed of simian virus 40 VP1 capsid protein. J Virol. 75:61-
72.
The Complete List of my Published Work can be found in My Bibliography:
http://www.ncbi.nlm.nih.gov/myncbi/collections/bibliography/50186865/?reload
D. RESEARCH SUPPORT
Patents:
1. Method of Inhibiting Non-sense mediated mRNA decay. United States Patent Application. Pub.
No. : US2011/0039911A1. Peery T, Mathews M, Hoque M, Hanauske et al
2. Alternative polyadenylation Isoforms as a Biomarker to determine the cell proliferation and
differentiation state (submitted). Luo W, Zhe Ji, Hoque M et al.
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