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Junying Yuan

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Nationality
  
American

Fields
  
Biology


Name
  
Junying Yuan

Junying Yuan StanfordNovartis Chemical Biology Seminar Series Junying Yuan PhD


Born
  
October 3, 1958 (age 65) Shanghai (
1958-10-03
)

Known for
  
Apoptosis research Necroptosis

Alma mater
  
Fudan University, Harvard University, Massachusetts Institute of Technology

Institution
  
Harvard Medical School

Institutions
  
Harvard Medical School

Doctoral advisor
  
H. Robert Horvitz

Junying Yuan (Chinese: 袁钧瑛; pinyin: Yuán Jūnyīng, born October 3, 1958) is the Elizabeth D. Hay Professor of Cell Biology at Harvard Medical School, best known for her work in cell death. Early in her career, she contributed significant findings to the discovery and characterization of apoptosis. More recently, she was responsible for the discovery of the programmed form of necrotic cell death known as necroptosis.

Contents

Junying Yuan Yuan Named Hay Professor of Cell Biology HMS

Education and early career

Junying Yuan Karolinska research lecture Junying Yuan The Nobel Prize in

Junying Yuan was born in Shanghai, her maternal grand father is the renowned professor and scholar Qingya Li (李青崖), who translated the famous French novels including Les Trois Mousquetaires and the complete work of Guy de Maupassant, and her paternal grandfather, Kaiji Yuan (袁开基) was a famous professor of organic chemistry. Her parents were both professors of medicine in Fudan University Shanghai Medical College, while her uncle, Chengye Yuan (袁承业), is a professor and a member (academician) of Chinese Academy of Sciences. Junying Yuan attended Fudan University following the revival of higher education after its suspension under the Cultural Revolution. She was among the first wave of students to attempt the newly revived National Higher Education Entrance Examination in 1977, coming in first of all students who attempted it in Shanghai. She completed her Bachelors in Biochemistry in 1982, and was subsequently one of the first students admitted to doctoral study in the United States through the China-U.S. Biochemistry Examination and Application (CUSBEA) program, coming in second out of the 25,000 who attempted the CUSBEA in its first year.

Junying Yuan Harvard Magazine

In the United States, she completed her PhD in Neuroscience(1989) at Harvard University under the supervision of MIT professor H. Robert Horvitz, where she endeavored to elucidate the molecular mechanisms behind programmed cell death in the nematode Caenorhabditis elegans. She identified the proteins ced-3 and ced-4 as drivers behind programmed cell death in C. elegans, and subsequently identified the mammalian homologue of ced-3 known as interleukin-1 beta-converting enzyme(ICE), later called caspase-1.

Career

Junying Yuan Lab Members Yuan Lab

Junying Yuan established an independent lab at Harvard-affiliated Massachusetts General Hospital in 1989, immediately upon completion of her PhD. Her initial efforts were directed towards providing evidence for the functional role of caspases in mediating mammalian apoptosis. Her independent work at this stage provided the first insights into molecular mechanisms in mammalian apoptosis, which contributed significantly to the Nobel Prize in Chemistry won by her PhD supervisor, Robert Horvitz.

Junying Yuan Junying Yuan PhD DFHCC

In 1996, Yuan moved her lab to the Department of Cell Biology at Harvard Medical School's Longwood campus, where she continued her investigation into cell death. Her work delved further into programmed cell death and revealed a wide cohort of proteins involved in the regulation and consequences of apoptosis. Some notable work includes her discovery that BID cleavage by caspase-8 mediates mitochondrial damage in apoptosis, and her discovery of caspase-11's role in regulating caspase-1-driven inflammation.

In 2005, Yuan's group discovered a non-apoptotic form of programmed necrotic cell death, which they termed "necroptosis". Other groups first observed that the stimulation of Fas/TNFR family of death-domain receptors(DR) activated a canonical apoptotic pathway; however, in many cell types, not only did caspase inhibition fail to inhibit cell death, as would be expected of canonical apoptosis, but stimulated cells experienced a form of cell death that more closely resembled necrosis than apoptosis. Yuan's group conducted a chemical screen that identified a small molecule capable of inhibiting DR-driven cell death, necrostatin-1, and demonstrated necroptosis' role in ischemic neuronal injury, thereby positing a potential role for necrostatin-1 in stroke treatment. Her group then identified RIPK1 as the target for necrostatin-1, thus implicating it as a key player in necroptosis. Yuan went on to identify and characterize members of the signaling network responsible for regulating necroptosis, and continues to elucidate the mechanisms of necroptosis while exploring its potential as a target of therapeutic intervention. Necrosis was previously considered to be a form of passive cell death, forced in response to stress. This belief had driven an aversion towards developing therapeutic applications targeting necrosis. In demonstrating a form of programmed necrosis, Yuan's work revealed new avenues of treatment for an ever-increasing cohort of diseases where necroptosis is implicated.

Awards and Fellowships

  • 1985-1989 Ryan Fellowship
  • 1994 Wilson S. Stone Memorial Award
  • 1996-1999 American Heart Established Investigator
  • 1999 SCBA Outstanding Young Investigator Award
  • 2002 Innovator Award for Breast Cancer Research
  • 2002 Merit Award, National Institute of Aging
  • 2003 BBS Mentoring Award, Harvard Medical School
  • 2005 National Institutes of Health Director's Pioneer Award
  • 2006 International Cell Death Society Award
  • 2007 Fellow of the American Academy of Arts and Sciences
  • 2010 Fellow of the American Association for the Advancement of Science
  • 2013 Agilent Technologies Thought Leader Award
  • 2017 Fellow of the National Academy of Sciences
  • References

    Junying Yuan Wikipedia


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