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Featured researches published by Yimin Yu.


Nature Chemical Biology | 2012

Pyruvate kinase M2 activators promote tetramer formation and suppress tumorigenesis

Dimitrios Anastasiou; Yimin Yu; William J. Israelsen; Jian Kang Jiang; Matthew B. Boxer; Bum Soo Hong; Wolfram Tempel; Svetoslav Dimov; Min Shen; Abhishek K. Jha; Hua Yang; Katherine R. Mattaini; Christian M. Metallo; Brian Prescott Fiske; Kevin D. Courtney; Scott Malstrom; Tahsin M. Khan; Charles Kung; Amanda P. Skoumbourdis; Henrike Veith; Noel Southall; Martin J. Walsh; Kyle R. Brimacombe; William Leister; Sophia Y. Lunt; Zachary R. Johnson; Katharine E. Yen; Kaiko Kunii; Shawn M. Davidson; Heather R. Christofk

Cancer cells engage in a metabolic program to enhance biosynthesis and support cell proliferation. The regulatory properties of pyruvate kinase M2 (PKM2) influence altered glucose metabolism in cancer. PKM2 interaction with phosphotyrosine-containing proteins inhibits enzyme activity and increases availability of glycolytic metabolites to support cell proliferation. This suggests that high pyruvate kinase activity may suppress tumor growth. We show that expression of PKM1, the pyruvate kinase isoform with high constitutive activity, or exposure to published small molecule PKM2 activators inhibit growth of xenograft tumors. Structural studies reveal that small molecule activators bind PKM2 at the subunit interaction interface, a site distinct from that of the endogenous activator fructose-1,6-bisphosphate (FBP). However, unlike FBP, binding of activators to PKM2 promotes a constitutively active enzyme state that is resistant to inhibition by tyrosine-phosphorylated proteins. These data support the notion that small molecule activation of PKM2 can interfere with anabolic metabolism.


Cell | 2013

PKM2 isoform-specific deletion reveals a differential requirement for pyruvate kinase in tumor cells.

William J. Israelsen; Talya L. Dayton; Shawn M. Davidson; Brian Prescott Fiske; Aaron M. Hosios; Gary Bellinger; Jie Li; Yimin Yu; Mika Sasaki; James W. Horner; Laura N. Burga; Jianxin Xie; Michael J. Jurczak; Ronald A. DePinho; Clary B. Clish; Tyler Jacks; Richard G. Kibbey; Gerburg Wulf; Dolores Di Vizio; Gordon B. Mills; Lewis C. Cantley; Matthew G. Vander Heiden

The pyruvate kinase M2 isoform (PKM2) is expressed in cancer and plays a role in regulating anabolic metabolism. To determine whether PKM2 is required for tumor formation or growth, we generated mice with a conditional allele that abolishes PKM2 expression without disrupting PKM1 expression. PKM2 deletion accelerated mammary tumor formation in a Brca1-loss-driven model of breast cancer. PKM2 null tumors displayed heterogeneous PKM1 expression, with PKM1 found in nonproliferating tumor cells and no detectable pyruvate kinase expression in proliferating cells. This suggests that PKM2 is not necessary for tumor cell proliferation and implies that the inactive state of PKM2 is associated with the proliferating cell population within tumors, whereas nonproliferating tumor cells require active pyruvate kinase. Consistent with these findings, variable PKM2 expression and heterozygous PKM2 mutations are found in human tumors. These data suggest that regulation of PKM2 activity supports the different metabolic requirements of proliferating and nonproliferating tumor cells.


Nature Chemical Biology | 2012

Erratum: Pyruvate kinase M2 activators promote tetramer formation and suppress tumorigenesis (Nature Chemical Biology (2012) 8 (839-847))

Dimitrios Anastasiou; Yimin Yu; William J. Israelsen; Jian Kang Jiang; Matthew B. Boxer; Bum Soo Hong; Wolfram Tempel; Svetoslav Dimov; Min Shen; Abhishek K. Jha; Hua Yang; Katherine R. Mattaini; Christian M. Metallo; Brian Prescott Fiske; Kevin D. Courtney; Scott Malstrom; Tahsin M. Khan; Charles Kung; Amanda P. Skoumbourdis; Henrike Veith; Noel Southall; Martin J. Walsh; Kyle R. Brimacombe; William Leister; Sophia Y. Lunt; Zachary R. Johnson; Katharine E. Yen; Kaiko Kunii; Shawn M. Davidson; Heather R. Christofk


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


PMC | 2013

PKM2 Isoform-Specific Deletion Reveals a Differential Requirement for Pyruvate Kinase in Tumor Cells

Jie Li; Mika Sasaki; James W. Horner; Laura N. Burga; Jianxin Xie; Michael J. Jurczak; Ronald A. DePinho; Clary B. Clish; Richard G. Kibbey; Gerburg Wulf; Dolores Di Vizio; Gordon B. Mills; Lewis C. Cantley; William J. Israelsen; Talya L. Dayton; Shawn M. Davidson; Brian Prescott Fiske; Aaron M. Hosios; Gary Bellinger; Yimin Yu; Tyler Jacks; Matthew G. Vander Heiden


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

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William J. Israelsen

Massachusetts Institute of Technology

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Henrike Veith

National Institutes of Health

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Hua Yang

Agios Pharmaceuticals

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Kyle R. Brimacombe

National Institutes of Health

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Martin J. Walsh

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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