Limited Environmental Serine and Glycine Confer Brain Metastasis Sensitivity to PHGDH Inhibition

Ngo, Bryan; Kim, E. D.; Osorio-Vasquez, Victoria; Doll, Sophia; Bustraan, Sophia; Liang, Roger J.; Luengo, Alba; Davidson, Shawn M.; Ali, Ahmed; Ferraro, Gino B.; Fischer, Grant M.; Eskandari, Roozbeh; Kang, Diane S.; Ni, Jing; Plasger, Ariana; Rajasekhar, Vinagolu K.; Kastenhuber, Edward R.; Bacha, Sarah; Sriram, Roshan K.; Stein, Benjamin D.; Bakhoum, Samuel F.; Snuderl, Matija; Cotzia, Paolo; Healey, John H.; Mainolfi, Nello; Suri, Vipin; Friedman, Adam; Manfredi, Mark; Sabatini, David M.; Jones, Drew R.; Yu, Min; Zhao, Jean J.; Jain, Rakesh K.; Keshari, Kayvan R.; Davies, Michael A.; Heiden, Matthew G. Vander; Hernando, Eva; Mann, Matthias; Cantley, Lewis C.; Pacold, Michael E.

doi:10.1158/2159-8290.cd-19-1228

Cited by 163 publications

(132 citation statements)

References 94 publications

Supporting

Mentioning

125

Contrasting

Order By: Relevance

“…While the combination of PH755 with a serine and glycine depleted diet could be beneficial in many cancer types, tumours arising in an environment naturally low in serine could benefit from PH755 treatment without the requirement for additional dietary intervention 23 . As shown recently, treatment with PH755 was effective in limiting serine synthesis and tumour growth of metastases in the brain, where environmental serine and glycine levels are low 31 . Furthermore, tumours carrying other genetic alterations that lead to resistance to dietary serine depletion, such as p53 or KRAS mutations, may be sensitive to the combination therapy described here.…”

Section: Discussionmentioning

confidence: 70%

“…More recently, a highly potent, selective and reversible PHGDH inhibitor, PH755, has been reported to prevent the flux of labelled glucose into serine in LPS stimulated macrophages and improve the survival of mice exposed to LPS-induced endotoxemia 30 . This inhibitor has also been shown to be effective to limit tumour growth in vivo 24 , 31 . In this study we examine the cooperation between serine and glycine starvation (-SG) and PHGDH inhibition (PHGDHi), demonstrating a reduction of tumour cell growth in vitro and in vivo.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Serine synthesis pathway inhibition cooperates with dietary serine and glycine limitation for cancer therapy

et al. 2021

Self Cite

View full text Add to dashboard Cite

Many tumour cells show dependence on exogenous serine and dietary serine and glycine starvation can inhibit the growth of these cancers and extend survival in mice. However, numerous mechanisms promote resistance to this therapeutic approach, including enhanced expression of the de novo serine synthesis pathway (SSP) enzymes or activation of oncogenes that drive enhanced serine synthesis. Here we show that inhibition of PHGDH, the first step in the SSP, cooperates with serine and glycine depletion to inhibit one-carbon metabolism and cancer growth. In vitro, inhibition of PHGDH combined with serine starvation leads to a defect in global protein synthesis, which blocks the activation of an ATF-4 response and more broadly impacts the protective stress response to amino acid depletion. In vivo, the combination of diet and inhibitor shows therapeutic efficacy against tumours that are resistant to diet or drug alone, with evidence of reduced one-carbon availability. However, the defect in ATF4-response seen in vitro following complete depletion of available serine is not seen in mice, where dietary serine and glycine depletion and treatment with the PHGDH inhibitor lower but do not eliminate serine. Our results indicate that inhibition of PHGDH will augment the therapeutic efficacy of a serine depleted diet.

show abstract

Section: Discussionmentioning

confidence: 70%

Section: Introductionmentioning

confidence: 99%

Serine synthesis pathway inhibition cooperates with dietary serine and glycine limitation for cancer therapy

et al. 2021

Self Cite

View full text Add to dashboard Cite

show abstract

“…The microenvironment of the brain is known to contain lower amounts of serine and glycine than the plasma [ 121 , 122 ]. Recently, PHGDH was shown to be a major determinant of brain metastasis in multiple human cancer types and preclinical models of breast cancer and melanoma ( Figure 6 A) [ 123 ]. In this particular study, genetic and pharmacological inhibition of PHGDH attenuated brain metastasis, indicating that PHGDH inhibitors may be useful in the treatment of brain metastasis [ 123 ].…”

Section: Metabolic Reprogramming To Form Metastatic Tumorsmentioning

confidence: 99%

Metabolic Reprogramming of Cancer Cells during Tumor Progression and Metastasis

Ohshima

Morii

2021

Metabolites

View full text Add to dashboard Cite

Cancer cells face various metabolic challenges during tumor progression, including growth in the nutrient-altered and oxygen-deficient microenvironment of the primary site, intravasation into vessels where anchorage-independent growth is required, and colonization of distant organs where the environment is distinct from that of the primary site. Thus, cancer cells must reprogram their metabolic state in every step of cancer progression. Metabolic reprogramming is now recognized as a hallmark of cancer cells and supports cancer growth. Elucidating the underlying mechanisms of metabolic reprogramming in cancer cells may help identifying cancer targets and treatment strategies. This review summarizes our current understanding of metabolic reprogramming during cancer progression and metastasis, including cancer cell adaptation to the tumor microenvironment, defense against oxidative stress during anchorage-independent growth in vessels, and metabolic reprogramming during metastasis.

show abstract

“…PHGDH has been demonstrated to be upregulated in a wide variety of biologically distinct cancers, including colorectal cancer [ 33 ] , gastric cancer [ 34 ] , breast cancer [ 35 , 36 ] , melanoma [ 37 ] , Ewing’s sarcoma [ 38 ] , cervical cancer [ 39 ] , pancreatic cancer [ 40 ] , thyroid cancer [ 41 ] , colon cancer [ 42 ] , lung adenocarcinoma [ 43 ] , and non-small cell lung cancer [ 44 ] . Furthermore, increased PHGDH expression has been linked to brain metastasis [ 45 ] .…”

Section: The Tumorigenic Consequences Of Elevated Phgdhmentioning

confidence: 99%

“…Furthermore, in a study in brain metastases, increased PHGDH expression was correlated with increased metastatic potential to the brain. Interestingly, in this study, inhibiting PHGDH attenuated metastasis without affecting extra-cranial tumour growth, suggesting that the consequences of increased PHGDH expression were directly related to upregulated metastasis [ 45 ] . Finally, this study highlighted the limited environmental availability of serine in the brain, demonstrating the subsequent reliance on de novo serine biosynthesis [ 45 ] .…”

Section: The Tumorigenic Consequences Of Elevated Phgdhmentioning

confidence: 99%

PHGDH as a mechanism for resistance in metabolically-driven cancers

Rathore

Schutt

Tine³

2020

CDR

View full text Add to dashboard Cite

At the forefront of cancer research is the rapidly evolving understanding of metabolic reprogramming within cancer cells. The expeditious adaptation to metabolic inhibition allows cells to evolve and acquire resistance to targeted treatments, which makes therapeutic exploitation complex but achievable. 3-phosphoglycerate dehydrogenase (PHGDH) is the rate-limiting enzyme of de novo serine biosynthesis and is highly expressed in a variety of cancers, including breast cancer, melanoma, and Ewing's sarcoma. This review will investigate the role of PHGDH in normal biological processes, leading to the role of PHGDH in the progression of cancer. With an understanding of the molecular mechanisms by which PHGDH expression advances cancer growth, we will highlight the known mechanisms of resistance to cancer therapeutics facilitated by PHGDH biology and identify avenues for combatting PHGDH-driven resistance with inhibitors of PHGDH to allow for the development of effective metabolic therapies.

show abstract

Limited Environmental Serine and Glycine Confer Brain Metastasis Sensitivity to PHGDH Inhibition

Cited by 163 publications

References 94 publications

Serine synthesis pathway inhibition cooperates with dietary serine and glycine limitation for cancer therapy

Serine synthesis pathway inhibition cooperates with dietary serine and glycine limitation for cancer therapy

Metabolic Reprogramming of Cancer Cells during Tumor Progression and Metastasis

PHGDH as a mechanism for resistance in metabolically-driven cancers

Contact Info

Product

Resources

About