Andrea Viczian profile picture
315 464-9494

Andrea Viczian博士

4613 Institute For Human Performance (IHP)
欧文大道505号
锡拉丘兹,纽约州13210
Andrea Viczian's email address generated as an image

CURRENT APPOINTMENTS

Associate Professor of Ophthalmology and Visual Sciences
Assistant Professor of Biochemistry and Molecular Biology
Assistant Professor of Cell and 发展al Biology
Assistant Professor of 神经科学 and Physiology

语言

英语

WEB资源

PUBMED
维兹安实验室网站
Center for Vision 研究

RESEARCH PROGRAMS AND AFFILIATIONS

Biochemistry and Molecular Biology
Biomedical Sciences Program
神经科学 and Physiology
神经科学项目
Ophthalmology and Visual Sciences

研究兴趣

Mammalian retinal stem cells formation; molecular mechanism of retinal cell fate decisions; vascular development in the CNS; using cell replacement therapy to heal the blinded eye.

ASSOCIATIONS / MEMBERSHIPS

Association for 研究 in Vision and Ophthalmology (ARVO)

教育

Postdoctoral Fellow: University of Cambridge, Cambridge, England, 2002, 发展al Biology
Postdoctoral Fellow: Marshall-Sherfield Fellow, University of Cambridge, 1999, 发展al Biology
博士: University of California at Los Angeles, 1998, 神经科学

研究抽象

研究

The eye develops in the anterior region of the embryonic neural plate and is one of the first organs to form. This region gives rise to the complex neural tissue, the retina. In blinding diseases like Age-Related Macular degeneration or Retinitis Pigmentosa, these light-sensing cells are lost and the human body cannot replace them. The Viczian team is interested in understanding the genes encoding transcription factors that drive the development of retina formation from pluripotent embryonic cells. In a 20+ year collaboration with the Zuber lab, our groups have been discovering the transcription factors and their roles in driving both of these processes. We use the relatively simple frog to better understand early eye formation (无花果. 1).

图1

We generate transgenic tadpoles to determine elements driving gene expression (无花果. 2).

图2

We use transplantation studies to determine transcription factors necessary and sufficient for eye formation (无花果. 3).

图3

We believe in group effort and we champion our trainees to discover the best of their abilities in performing their research. Our current work has transitioned from using frog to knockout mouse studies and embryonic stem cell cultures to determine conservation of gene function from frog to mouse. We look forward to you joining us in this supportive, yet exciting, environment.

Graduate studies in the Viczian lab. 学生 interested in joining the Viczian lab are welcome to email Dr. Viczian to discuss shared research interests.

Selected publications

Ledford K. L., Martinez-De Luna, R. I.泰森,M. A.罗林斯,K. D.维兹安,A. S.和M . Zuber. E. (2017). Distinct cis-acting regions control six6 expression during eye field and optic cup stages of eye formation. 开发生物 426, 418-428.

Motahari Z., Martinez-De Luna, R. I.维兹安,A. S.和M . Zuber. E. (2016). Tbx3 represses bmp4 expression and with Pax6 is required and sufficient for retina formation. 发展 143, 3560-3572.

Wong K. A.特伦布利,M.Abd Wahab, S.Viczian,. S. (2015). Efficient retina formation requires suppression of both Activin and BMP signaling pathways in pluripotent cells. 开放杂志 4, 573-583.

Viczian,. S. (2013). Advances in retinal stem cell biology. [J]眼科 8, 147-159.

Viczian,. S.索莱西奥,E. C.,你,Y.和M . Zuber. E. (2009). Generation of functional eyes from pluripotent cells. 公共科学图书馆杂志 7, e1000174.

出版物

链接到 PubMed (打开新窗口. 关闭 the PubMed window to return to this page.)