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Dive into the research topics where Hee-Won Park is active.

Publication


Featured researches published by Hee-Won Park.


Bioorganic & Medicinal Chemistry Letters | 2010

Evaluation of thieno[3,2-b]pyrrole[3,2-d]pyridazinones as activators of the tumor cell specific M2 isoform of pyruvate kinase

Jian-kang Jiang; Matthew B. Boxer; Matthew G. Vander Heiden; Min Shen; Amanda P. Skoumbourdis; Noel Southall; Henrike Veith; William Leister; Christopher P. Austin; Hee-Won Park; James Inglese; Lewis C. Cantley; Douglas S. Auld; Craig J. Thomas

Cancer cells have distinct metabolic needs that are different from normal cells and can be exploited for development of anti-cancer therapeutics. Activation of the tumor specific M2 form of pyruvate kinase (PKM2) is a potential strategy for returning cancer cells to a metabolic state characteristic of normal cells. Here, we describe activators of PKM2 based upon a substituted thieno[3,2-b]pyrrole[3,2-d]pyridazinone scaffold. The synthesis of these agents, structure-activity relationships, analysis of activity at related targets (PKM1, PKR and PKL) and examination of aqueous solubility are investigated. These agents represent the second reported chemotype for activation of PKM2.


Archive | 2013

ML265: A potent PKM2 activator induces tetramerization and reduces tumor formation and size in a mouse xenograft model

Martin J. Walsh; Kyle R. Brimacombe; Dimitrios Anastasiou; Yimin Yu; William J. Israelsen; Bum-Soo Hong; Wolfram Tempel; Svetoslav Dimov; Henrike Veith; Hua Yang; Charles Kung; Katharine E. Yen; Lenny Dang; Francesco G. Salituro; Douglas S. Auld; Hee-Won Park; Matthew G. Vander Heiden; Craig J. Thomas; Min Shen; Matthew B. Boxer


Archive | 2013

ML285 affects reactive oxygen species’ inhibition of pyruvate kinase M2

Kyle R. Brimacombe; Dimitrios Anastasiou; Bum-Soo Hong; Wolfram Tempel; Svetoslav Dimov; Henrike Veith; Douglas S. Auld; Matthew G. Vander Heiden; Craig J. Thomas; Hee-Won Park; Min Shen; Lewis C. Cantley; Matthew B. Boxer


Archive | 2013

Table 2, In vitro ADME profile for ML202 and ML265

Martin J. Walsh; Kyle R. Brimacombe; Dimitrios Anastasiou; Yimin Yu; William J. Israelsen; Bum-Soo Hong; Wolfram Tempel; Svetoslav Dimov; Henrike Veith; Hua Yang; Charles Kung; Katharine E. Yen; Lenny Dang; Francesco G. Salituro; Douglas S. Auld; Hee-Won Park; Matthew G. Vander Heiden; Craig J. Thomas; Min Shen; Matthew B. Boxer


Archive | 2013

Table 1, Extended probe submitted to the MLSMR

Martin J. Walsh; Kyle R. Brimacombe; Dimitrios Anastasiou; Yimin Yu; William J. Israelsen; Bum-Soo Hong; Wolfram Tempel; Svetoslav Dimov; Henrike Veith; Hua Yang; Charles Kung; Katharine E. Yen; Lenny Dang; Francesco G. Salituro; Douglas S. Auld; Hee-Won Park; Matthew G. Vander Heiden; Craig J. Thomas; Min Shen; Matthew B. Boxer


Archive | 2013

Figure 1, Previous PKM2 activator ML probes

Martin J. Walsh; Kyle R. Brimacombe; Dimitrios Anastasiou; Yimin Yu; William J. Israelsen; Bum-Soo Hong; Wolfram Tempel; Svetoslav Dimov; Henrike Veith; Hua Yang; Charles Kung; Katharine E. Yen; Lenny Dang; Francesco G. Salituro; Douglas S. Auld; Hee-Won Park; Matthew G. Vander Heiden; Craig J. Thomas; Min Shen; Matthew B. Boxer


Archive | 2013

Figure 8, [a) Size exclusion chromatography was...].

Martin J. Walsh; Kyle R. Brimacombe; Dimitrios Anastasiou; Yimin Yu; William J. Israelsen; Bum-Soo Hong; Wolfram Tempel; Svetoslav Dimov; Henrike Veith; Hua Yang; Charles Kung; Katharine E. Yen; Lenny Dang; Francesco G. Salituro; Douglas S. Auld; Hee-Won Park; Matthew G. Vander Heiden; Craig J. Thomas; Min Shen; Matthew B. Boxer


Archive | 2013

Figure 4, ML265 activates PKM2 in the presence of phosphorylated peptides

Martin J. Walsh; Kyle R. Brimacombe; Dimitrios Anastasiou; Yimin Yu; William J. Israelsen; Bum-Soo Hong; Wolfram Tempel; Svetoslav Dimov; Henrike Veith; Hua Yang; Charles Kung; Katharine E. Yen; Lenny Dang; Francesco G. Salituro; Douglas S. Auld; Hee-Won Park; Matthew G. Vander Heiden; Craig J. Thomas; Min Shen; Matthew B. Boxer


Archive | 2013

Figure 7, PKM2 activation (scaled from initial velocities) as a function of a) PEP and b) ADP concentration in the presence of 10μM 1,6-FBP (gray circles), ML265 (black circles) or DMSO control (white circles)

Martin J. Walsh; Kyle R. Brimacombe; Dimitrios Anastasiou; Yimin Yu; William J. Israelsen; Bum-Soo Hong; Wolfram Tempel; Svetoslav Dimov; Henrike Veith; Hua Yang; Charles Kung; Katharine E. Yen; Lenny Dang; Francesco G. Salituro; Douglas S. Auld; Hee-Won Park; Matthew G. Vander Heiden; Craig J. Thomas; Min Shen; Matthew B. Boxer


Archive | 2013

Figure 6, H1299 cells incubated with 50 μM ML265 for 1 hour, lysed followed by 2-D electrophoresis, Western blot and PGAM1 antibody staining

Martin J. Walsh; Kyle R. Brimacombe; Dimitrios Anastasiou; Yimin Yu; William J. Israelsen; Bum-Soo Hong; Wolfram Tempel; Svetoslav Dimov; Henrike Veith; Hua Yang; Charles Kung; Katharine E. Yen; Lenny Dang; Francesco G. Salituro; Douglas S. Auld; Hee-Won Park; Matthew G. Vander Heiden; Craig J. Thomas; Min Shen; Matthew B. Boxer

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Craig J. Thomas

National Institutes of Health

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Douglas S. Auld

National Institutes of Health

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Henrike Veith

National Institutes of Health

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Matthew B. Boxer

National Institutes of Health

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Matthew G. Vander Heiden

Massachusetts Institute of Technology

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Min Shen

National Institutes of Health

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Kyle R. Brimacombe

National Institutes of Health

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Hua Yang

Agios Pharmaceuticals

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