Guomao Zhao
Nationwide Children's Hospital
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Publication
Featured researches published by Guomao Zhao.
Placenta | 2016
William E. Ackerman; Irina Buhimschi; Haley R. Eidem; David C. Rinker; Antonis Rokas; Kara Rood; Guomao Zhao; Taryn Summerfield; Mark B. Landon; Catalin S. Buhimschi
INTRODUCTIONnWe performed RNA sequencing with the primary goal of discovering key placental villous trophoblast (VT) and decidua basalis (DB) transcripts differentially expressed in intra-amniotic infection (IAI)-induced preterm birth (PTB).nnnMETHODSnRNA was extracted from 15 paired VT and DB specimens delivered of women with: 1) spontaneous PTB in the setting of amniocentesis-proven IAI and histological chorioamnionitis (nxa0=xa05); 2) spontaneous idiopathic PTB (iPTB, nxa0=xa05); and 3) physiologic term pregnancy (nxa0=xa05). RNA sequencing was performed using the Illumina HiSeq 2500 platform, and a spectrum of computational tools was used for gene prioritization and pathway analyses.nnnRESULTSnIn the VT specimens, 128 unique long transcripts and 7 mature microRNAs differed significantly between pregnancies complicated by IAI relative to iPTB (FDR<0.1). The up-regulated transcripts included many characteristic of myeloblast-derived cells, and bioinformatic analyses revealed enrichment for multiple pathways associated with acute inflammation. In an expanded cohort including additional IAI and iPTB specimens, the expression of three proteins (cathepsin S, lysozyme, and hexokinase 3) and two microRNAs (miR-133a and miR-223) was validated using immunohistochemistry and quantitative PCR, respectively. In the DB specimens, only 11 long transcripts and no microRNAs differed significantly between IAI cases and iPTB controls (FDR<0.1). Comparison of the VT and DB specimens in each clinical scenario revealed signatures distinguishing these placental regions.nnnDISCUSSIONnIAI is associated with a transcriptional signature consistent with acute inflammation in the villous trophoblast. The present findings illuminate novel signaling pathways involved in IAI, and suggest putative therapeutic targets and potential biomarkers associated with this condition.
American Journal of Obstetrics and Gynecology | 2017
William Ackerman; Irina A. Buhimschi; Taryn Summerfield; Guomao Zhao; Mark B. Landon; Catalin S. Buhimschi
American Journal of Obstetrics and Gynecology | 2017
Megan Jones; Irina A. Buhimschi; Guomao Zhao; Anna Bartholomew; Jordan Smith; Aubry Fowler; Stephen Thung; Kara Rood; Catalin S. Buhimschi
American Journal of Obstetrics and Gynecology | 2017
Kara Rood; Irina A. Buhimschi; Guomao Zhao; Stacy Beck; Michael Cackovic; Mert Ozan Bahtyiar; Taryn Summerfield; Megan Locke; Catalin S. Buhimschi
American Journal of Obstetrics and Gynecology | 2017
William Ackerman; Kathy Cordova; Megan Locke; Taryn Summerfield; Guomao Zhao; Catalin S. Buhimschi; Irina A. Buhimschi
American Journal of Obstetrics and Gynecology | 2017
Guomao Zhao; Emily A. Oliver; Kara Rood; Catalin S. Buhimschi; Taryn Summerfield; Irina A. Buhimschi
American Journal of Obstetrics and Gynecology | 2017
Kathryn Berryman; Catalin S. Buhimschi; Guomao Zhao; Michelle Axe; Megan Locke; Irina A. Buhimschi
American Journal of Obstetrics and Gynecology | 2017
Brian Kellert; Bethany T. Stetson; Min Li; Hanaa Motawea; Guomao Zhao; Megan Locke; Catalin S. Buhimschi; Irina A. Buhimschi
American Journal of Obstetrics and Gynecology | 2017
Brian Kellert; Bethany T. Stetson; Guomao Zhao; Min Li; Hanaa Motawea; Catalin S. Buhimschi; Irina A. Buhimschi
American Journal of Obstetrics and Gynecology | 2016
William E. Ackerman; Irina Buhimschi; Guomao Zhao; Taryn Summerfield; Hongwu Jing; Catalin S. Buhimschi