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Dive into the research topics where Yijia Liu is active.

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Featured researches published by Yijia Liu.


Nature Medicine | 2005

Using siRNA in prophylactic and therapeutic regimens against SARS coronavirus in Rhesus macaque

Bao-Jian Li; Qingquan Tang; Du Cheng; Chuan Qin; Frank Y. Xie; Qiang Wei; Jun Xu; Yijia Liu; Bo-Jian Zheng; Martin C. Woodle; Nanshan Zhong; Patrick Y. Lu

Development of therapeutic agents for severe acute respiratory syndrome (SARS) viral infection using short interfering RNA (siRNA) inhibitors exemplifies a powerful new means to combat emerging infectious diseases. Potent siRNA inhibitors of SARS coronavirus (SCV) in vitro were further evaluated for efficacy and safety in a rhesus macaque (Macaca mulatta) SARS model using clinically viable delivery while comparing three dosing regimens. Observations of SARS-like symptoms, measurements of SCV RNA presence and lung histopathology and immunohistochemistry consistently showed siRNA-mediated anti-SARS efficacy by either prophylactic or therapeutic regimens. The siRNAs used provided relief from SCV infection–induced fever, diminished SCV viral levels and reduced acute diffuse alveoli damage. The 10–40 mg/kg accumulated dosages of siRNA did not show any sign of siRNA-induced toxicity. These results suggest that a clinical investigation is warranted and illustrate the prospects for siRNA to enable a massive reduction in development time for new targeted therapeutic agents.


PLOS Neglected Tropical Diseases | 2011

Polyethyleneimine (PEI) Mediated siRNA Gene Silencing in the Schistosoma mansoni Snail Host, Biomphalaria glabrata

Matty Knight; Andre Miller; Yijia Liu; Puthupparampil V. Scaria; Martin C. Woodle; Wannaporn Ittiprasert

An in vivo, non-invasive technique for gene silencing by RNA interference (RNAi) in the snail, Biomphalaria glabrata, has been developed using cationic polymer polyethyleneimine (PEI) mediated delivery of long double-stranded (ds) and small interfering (si) RNA. Cellular delivery was evaluated and optimized by using a ‘mock’ fluorescent siRNA. Subsequently, we used the method to suppress expression of Cathepsin B (CathB) with either the corresponding siRNA or dsRNA of this transcript. In addition, the knockdown of peroxiredoxin (Prx) at both RNA and protein levels was achieved with the PEI-mediated soaking method. B. glabrata is an important snail host for the transmission of the parasitic digenean platyhelminth, Schistosoma mansoni that causes schistosomiasis in the neotropics. Progress is being made to realize the genome sequence of the snail and to uncover gene expression profiles and cellular pathways that enable the snail to either prevent or sustain an infection. Using PEI complexes, a convenient soaking method has been developed, enabling functional gene knockdown studies with either dsRNA or siRNA. The protocol developed offers a first whole organism method for host-parasite gene function studies needed to identify key mechanisms required for parasite development in the snail host, which ultimately are needed as points for disrupting this parasite mediated disease.


Journal of Drug Targeting | 2014

Enhancement of antifungal activity by integrin-targeting of branched histidine rich peptides

Puthupparampil V. Scaria; Yijia Liu; Qixin Leng; Szu-Ting Chou; A. James Mixson; Martin C. Woodle

Abstract The treatment of invasive candidiasis associated with growing numbers of immunocompromised patients remains a major challenge complicated by increasing drug resistance. A novel class of branched histidine-lysine (bHK) peptides has promising antifungal activity, and exhibits a mechanism similar to natural histatins, and thus may avoid drug resistance. The present studies evaluate ligand targeting of bHK peptides to fungal surface integrins by determining whether a cyclic RGD (cRGD) peptide with a large PEG linker could enhance bHK peptide antifungal activity. Whereas conjugates containing only the PEG linker reduced bHK peptide activity, conjugates with the cRGD-PEG ligand resulted in marked enhancement of activity against Candida albicans. This study provides the first demonstration of benefit from ligand targeting of antifungal agents to fungal surface receptors.


Archive | 2007

COMPOSITION AND METHODS OF RNAi THERAPEUTICS FOR TREATMENT OF CANCER AND OTHER NEOVASCULARIZATION DISEASES

Yijia Liu; Patrick Y. Lu; Martin C. Woodle; Frank Y. Xie


Oncotarget | 2014

Systemic miRNA-7 delivery inhibits tumor angiogenesis and growth in murine xenograft glioblastoma

Negar Babae; Meriem Bourajjaj; Yijia Liu; Judy R. van Beijnum; Francesco Cerisoli; Puthupparampil V. Scaria; Mark Verheul; Maaike P. Van Berkel; Ebel H.E. Pieters; Rick J. van Haastert; Afrouz Yousefi; Enrico Mastrobattista; Gert Storm; Eugene Berezikov; Edwin Cuppen; Martin C. Woodle; Roel Q. J. Schaapveld; Grégoire Pierre André Prevost; Arjan W. Griffioen; Paula I. van Noort; Raymond M. Schiffelers


Archive | 2004

TARGETS FOR TUMOR GROWTH INHIBITION

Patrick Y. Lu; Frank Y. Xie; Martin C. Woodle; Yijia Liu; Quinn Tang; Jun Xu


Archive | 2006

COMPOSITIONS AND METHODS OF USING siRNA TO KNOCKDOWN GENE EXPRESSION AND TO IMPROVE SOLID ORGAN AND CELL TRANSPLANTATION

Marie Denise Parker; Julian R. Pratt; Yijia Liu; Yang Lu; Martin Woodle; Yuefeng Xie


Archive | 2006

Inhibitory polynucleotide compositions and methods for treating cancer

Frank Y. Xie; Patrick Y. Lu; Martin C. Woodle; Yijia Liu


Archive | 2004

Rnai agents for anti-sars coronavirus therapy

Quinn Tang; Patrick Y. Lu; Frank Y. Xie; Yijia Liu; Jun Xu; Martin C. Woodle


Archive | 2008

Compositions comprising human egfr-sirna and methods of use

Xiaodong Yang; Frank Y. Xie; Yijia Liu; Ying Liu

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Qixin Leng

University of Maryland

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Matty Knight

George Washington University

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