Zobrazeno 1 - 10
of 14
pro vyhledávání: '"Megan, Priston"'
Autor:
Tianhua Huang, PhD, Shamim Rashid, BSc, Megan Priston, MS, Evasha Rasasakaram, MS, Ellen Mak-Tam, BSc, Clare Gibbons, MS, Elad Mei-Dan, MD, H. Melanie Bedford, MD
Publikováno v:
AJOG Global Reports, Vol 3, Iss 2, Pp 100193- (2023)
BACKGROUND: Professional societies have recommended universal first trimester screening for preeclampsia and a second or third trimester soluble fms-like tyrosine kinase-1–placental growth factor ratio test to assess for preeclampsia and its severi
Externí odkaz:
https://doaj.org/article/9254205448d64ea9ab6b868716ca4292
Autor:
Tianhua Huang, H. Melanie Bedford, Shamim Rashid, Evasha Rasasakaram, Megan Priston, Ellen Mak-Tam, Clare Gibbons, Wendy S. Meschino, Howard Cuckle, Elad Mei-Dan
Publikováno v:
BMC Pregnancy and Childbirth, Vol 22, Iss 1, Pp 1-14 (2022)
Abstract Background Abnormal levels of maternal biochemical markers used in multiple marker aneuploidy screening have been associated with adverse pregnancy outcomes. This study aims to assess if a combination of maternal characteristics and biochemi
Externí odkaz:
https://doaj.org/article/6296fe0375c74458a6a421fe71e136cc
Autor:
Tianhua Huang, H. Melanie Bedford, Shamim Rashid, Evasha Rasasakaram, Megan Priston, Ellen Mak-Tam, Clare Gibbons, Wendy S. Meschino, Howard Cuckle, Elad Mei-Dan
Publikováno v:
BMC pregnancy and childbirth. 22(1)
Background Abnormal levels of maternal biochemical markers used in multiple marker aneuploidy screening have been associated with adverse pregnancy outcomes. This study aims to assess if a combination of maternal characteristics and biochemical marke
Autor:
Tianhua Huang, Shamim Rashid, Alan Dennis, Ellen Mak-Tam, Megan Priston, Clare Gibbons, Melanie Bedford, Wendy Meschino, Howard Cuckle, Elad Mei-Dan
Publikováno v:
American Journal of Obstetrics and Gynecology. 226:S638
Autor:
Tianhua Huang, Shamim Rashid, Ellen Mak-Tam, Megan Priston, Clare Gibbons, Melanie Bedford, Elad Mei-Dan
Publikováno v:
American Journal of Obstetrics and Gynecology. 226:S338
Autor:
Dan Gill, Yvonne M. Buys, Elise Heon, Mike A. Walter, Megan Priston, Kathy Kozlowski, Ken Letwin, Alex V. Levin
Publikováno v:
Human Molecular Genetics. 10:1631-1638
The specific role of PITX2 in the pathogenesis of anterior segment dysgenesis has yet to be clearly defined. We provide here new insight into PITX2 pathogenesis through mutational and functional analyses. Three PITX2 mutations were found in a screen
Publikováno v:
Journal of Medical Genetics. 37:422-427
Glaucoma is a leading cause of irreversible blindness in Canada. Congenital glaucoma usually manifests during the first years of life and is characterised by severe visual loss and autosomal recessive inheritance. Two disease loci, on chromosomes 1p3
Autor:
Elise Héon, Philippe Othenin Girard, Gail Billingsley, Nicolette H. Lubsen, Daniel F. Schorderet, Megan Priston, Francis L. Munier
Publikováno v:
The American Journal of Human Genetics. 65:1261-1267
Despite the fact that cataracts constitute the leading cause of blindness worldwide, the mechanisms of lens opacification remain unclear. We recently mapped the aculeiform cataract to the gamma-crystallin locus (CRYG) on chromosome 2q33-35, and mutat
Autor:
Andrea, Vincent, Gail, Billingsley, Megan, Priston, Tom, Glaser, Edward, Oliver, Mike, Walter, Robert, Ritch, Alex, Levin, Elise, Heon
Publikováno v:
Molecular vision. 12
Peters anomaly is a developmental anomaly of the eye frequently associated with glaucoma. The aim of this study was to further define the molecular basis of this condition.The role of four candidate genes implicated in ocular development or glaucoma,
Autor:
Colin E, Willoughby, Ayad, Shafiq, Walter, Ferrini, Louie Loh Yen, Chan, Gail, Billingsley, Megan, Priston, Calvin, Mok, Arvind, Chandna, Stephen, Kaye, Elise, Héon
Publikováno v:
Molecular vision. 11
The molecular characterization of a UK family with an autosomal dominant congenital cataract associated with microcornea is reported.Family history and clinical data were recorded. This phenotype was linked to a 7.6 cM region of chromosome 22q11.2-q1