Depleted hexokinase1 and lack of AMPKα activation favor OXPHOS-dependent energetics in retinoblastoma tumors

Vishnu Suresh Babu; Ashwin Mallipatna; Gagan Dudeja; Rohit Shetty; Archana Padmanabhan Nair; Sai Bo Bo Tun; Candice Ee Hua Ho; Shyam S. Chaurasia; Shomi S. Bhattacharya; Navin Kumar Verma; Rajamani Lakshminarayanan; Nilanjan Guha; Stephane Heymans; Veluchamy Amutha Barathi; Arkasubhra Ghosh

doi:10.1016/j.trsl.2023.07.001

Depleted hexokinase1 and lack of AMPKα activation favor OXPHOS-dependent energetics in retinoblastoma tumors

Vishnu Suresh Babu, Ashwin Mallipatna, Gagan Dudeja, Rohit Shetty, Archana Padmanabhan Nair, Sai Bo Bo Tun, Candice Ee Hua Ho, Shyam S. Chaurasia, Shomi S. Bhattacharya, Navin Kumar Verma, Rajamani Lakshminarayanan, Nilanjan Guha, Stephane Heymans, Veluchamy Amutha Barathi, Arkasubhra Ghosh^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Lack of retinoblastoma (Rb) protein causes aggressive intraocular retinal tumors in children. Recently, Rb tumors have been shown to have a distinctly altered metabolic phenotype, such as reduced expression of glycolytic pathway proteins alongside altered pyruvate and fatty acid levels. In this study, we demonstrate that loss of hexokinase 1(HK1) in tumor cells rewires their metabolism allowing enhanced oxidative phosphorylation-dependent energy production. We show that rescuing HK1 or retinoblastoma protein 1 (RB1) in these Rb cells reduced cancer hallmarks such as proliferation, invasion, and spheroid formation and increased their sensitivity to chemotherapy drugs. Induction of HK1 was accompanied by a metabolic shift of the cells to glycolysis and a reduction in mitochondrial mass. Cytoplasmic HK1 bound Liver Kinase B1 and phosphorylated AMP-activated kinase-a (AMPKa Thr172), thereby reducing mitochondria-dependent energy production. We validated these findings in tumor samples from Rb patients compared to age-matched healthy retinae. HK1 or RB1 expression in Rb-/- cells led to a reduction in their respiratory capacity and glycolytic proton flux. HK1 overexpression reduced tumor burden in an intraocular tumor xenograft model. AMPKa activation by AICAR also enhanced the tumoricidal effects of the chemotherapeutic drug topotecan in vivo. Therefore, enhancing HK1 or AMPKa activity can reprogram cancer metabolism and sensitize Rb tumors to lower doses of existing treatments, a potential therapeutic modality for Rb.

Original language	English
Pages (from-to)	41-56
Number of pages	16
Journal	Translational Research
Volume	261
Issue number	1
Early online date	6 Jun 2023
DOIs	https://doi.org/10.1016/j.trsl.2023.07.001
Publication status	Published - Nov 2023

Keywords

AMPKa
Cancer
Glycolysis
Hexokinase-1
Oxidative phosphorylation
Retinoblastoma

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10.1016/j.trsl.2023.07.001

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Babu, V. S., Mallipatna, A., Dudeja, G., Shetty, R., Nair, A. P., Tun, S. B. B., Ho, C. E. H., Chaurasia, S. S., Bhattacharya, S. S., Verma, N. K., Lakshminarayanan, R., Guha, N., Heymans, S., Barathi, V. A., & Ghosh, A. (2023). Depleted hexokinase1 and lack of AMPKα activation favor OXPHOS-dependent energetics in retinoblastoma tumors. Translational Research, 261(1), 41-56. https://doi.org/10.1016/j.trsl.2023.07.001

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title = "Depleted hexokinase1 and lack of AMPKα activation favor OXPHOS-dependent energetics in retinoblastoma tumors",

abstract = "Lack of retinoblastoma (Rb) protein causes aggressive intraocular retinal tumors in children. Recently, Rb tumors have been shown to have a distinctly altered metabolic phenotype, such as reduced expression of glycolytic pathway proteins alongside altered pyruvate and fatty acid levels. In this study, we demonstrate that loss of hexokinase 1(HK1) in tumor cells rewires their metabolism allowing enhanced oxidative phosphorylation-dependent energy production. We show that rescuing HK1 or retinoblastoma protein 1 (RB1) in these Rb cells reduced cancer hallmarks such as proliferation, invasion, and spheroid formation and increased their sensitivity to chemotherapy drugs. Induction of HK1 was accompanied by a metabolic shift of the cells to glycolysis and a reduction in mitochondrial mass. Cytoplasmic HK1 bound Liver Kinase B1 and phosphorylated AMP-activated kinase-a (AMPKa Thr172), thereby reducing mitochondria-dependent energy production. We validated these findings in tumor samples from Rb patients compared to age-matched healthy retinae. HK1 or RB1 expression in Rb-/- cells led to a reduction in their respiratory capacity and glycolytic proton flux. HK1 overexpression reduced tumor burden in an intraocular tumor xenograft model. AMPKa activation by AICAR also enhanced the tumoricidal effects of the chemotherapeutic drug topotecan in vivo. Therefore, enhancing HK1 or AMPKa activity can reprogram cancer metabolism and sensitize Rb tumors to lower doses of existing treatments, a potential therapeutic modality for Rb.",

keywords = "AMPKa, Cancer, Glycolysis, Hexokinase-1, Oxidative phosphorylation, Retinoblastoma",

author = "Babu, {Vishnu Suresh} and Ashwin Mallipatna and Gagan Dudeja and Rohit Shetty and Nair, {Archana Padmanabhan} and Tun, {Sai Bo Bo} and Ho, {Candice Ee Hua} and Chaurasia, {Shyam S.} and Bhattacharya, {Shomi S.} and Verma, {Navin Kumar} and Rajamani Lakshminarayanan and Nilanjan Guha and Stephane Heymans and Barathi, {Veluchamy Amutha} and Arkasubhra Ghosh",

note = "Funding Information: Conflicts of Interest: SH receives personal fees for scientific advice to Astra-Zeneca, Cellprothera and Merck; unrestricted research grant from Pfizer, outside the content of this work. The other authors have no competing interests. Funding Information: The authors thank Narayana Nethralaya Foundation for funding research support to V.S.B, A.P.N, R.K, A.G. Research internship of V.S.B in NKV lab was supported by NKV's Start-Up Grant, LKC Medicine, Nanyang Technological University Singapore ( L0412290 ). The funders had no role in design, data collection, analysis, decision to publish, or preparation of the manuscript. Publisher Copyright: {\textcopyright} 2023 Elsevier Inc.",

year = "2023",

month = nov,

doi = "10.1016/j.trsl.2023.07.001",

language = "English",

volume = "261",

pages = "41--56",

journal = "Translational Research",

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Babu, VS, Mallipatna, A, Dudeja, G, Shetty, R, Nair, AP, Tun, SBB, Ho, CEH, Chaurasia, SS, Bhattacharya, SS, Verma, NK, Lakshminarayanan, R, Guha, N, Heymans, S, Barathi, VA & Ghosh, A 2023, 'Depleted hexokinase1 and lack of AMPKα activation favor OXPHOS-dependent energetics in retinoblastoma tumors', Translational Research, vol. 261, no. 1, pp. 41-56. https://doi.org/10.1016/j.trsl.2023.07.001

TY - JOUR

T1 - Depleted hexokinase1 and lack of AMPKα activation favor OXPHOS-dependent energetics in retinoblastoma tumors

AU - Babu, Vishnu Suresh

AU - Mallipatna, Ashwin

AU - Dudeja, Gagan

AU - Shetty, Rohit

AU - Nair, Archana Padmanabhan

AU - Tun, Sai Bo Bo

AU - Ho, Candice Ee Hua

AU - Chaurasia, Shyam S.

AU - Bhattacharya, Shomi S.

AU - Verma, Navin Kumar

AU - Lakshminarayanan, Rajamani

AU - Guha, Nilanjan

AU - Heymans, Stephane

AU - Barathi, Veluchamy Amutha

AU - Ghosh, Arkasubhra

N1 - Funding Information: Conflicts of Interest: SH receives personal fees for scientific advice to Astra-Zeneca, Cellprothera and Merck; unrestricted research grant from Pfizer, outside the content of this work. The other authors have no competing interests. Funding Information: The authors thank Narayana Nethralaya Foundation for funding research support to V.S.B, A.P.N, R.K, A.G. Research internship of V.S.B in NKV lab was supported by NKV's Start-Up Grant, LKC Medicine, Nanyang Technological University Singapore ( L0412290 ). The funders had no role in design, data collection, analysis, decision to publish, or preparation of the manuscript. Publisher Copyright: © 2023 Elsevier Inc.

PY - 2023/11

Y1 - 2023/11

N2 - Lack of retinoblastoma (Rb) protein causes aggressive intraocular retinal tumors in children. Recently, Rb tumors have been shown to have a distinctly altered metabolic phenotype, such as reduced expression of glycolytic pathway proteins alongside altered pyruvate and fatty acid levels. In this study, we demonstrate that loss of hexokinase 1(HK1) in tumor cells rewires their metabolism allowing enhanced oxidative phosphorylation-dependent energy production. We show that rescuing HK1 or retinoblastoma protein 1 (RB1) in these Rb cells reduced cancer hallmarks such as proliferation, invasion, and spheroid formation and increased their sensitivity to chemotherapy drugs. Induction of HK1 was accompanied by a metabolic shift of the cells to glycolysis and a reduction in mitochondrial mass. Cytoplasmic HK1 bound Liver Kinase B1 and phosphorylated AMP-activated kinase-a (AMPKa Thr172), thereby reducing mitochondria-dependent energy production. We validated these findings in tumor samples from Rb patients compared to age-matched healthy retinae. HK1 or RB1 expression in Rb-/- cells led to a reduction in their respiratory capacity and glycolytic proton flux. HK1 overexpression reduced tumor burden in an intraocular tumor xenograft model. AMPKa activation by AICAR also enhanced the tumoricidal effects of the chemotherapeutic drug topotecan in vivo. Therefore, enhancing HK1 or AMPKa activity can reprogram cancer metabolism and sensitize Rb tumors to lower doses of existing treatments, a potential therapeutic modality for Rb.

AB - Lack of retinoblastoma (Rb) protein causes aggressive intraocular retinal tumors in children. Recently, Rb tumors have been shown to have a distinctly altered metabolic phenotype, such as reduced expression of glycolytic pathway proteins alongside altered pyruvate and fatty acid levels. In this study, we demonstrate that loss of hexokinase 1(HK1) in tumor cells rewires their metabolism allowing enhanced oxidative phosphorylation-dependent energy production. We show that rescuing HK1 or retinoblastoma protein 1 (RB1) in these Rb cells reduced cancer hallmarks such as proliferation, invasion, and spheroid formation and increased their sensitivity to chemotherapy drugs. Induction of HK1 was accompanied by a metabolic shift of the cells to glycolysis and a reduction in mitochondrial mass. Cytoplasmic HK1 bound Liver Kinase B1 and phosphorylated AMP-activated kinase-a (AMPKa Thr172), thereby reducing mitochondria-dependent energy production. We validated these findings in tumor samples from Rb patients compared to age-matched healthy retinae. HK1 or RB1 expression in Rb-/- cells led to a reduction in their respiratory capacity and glycolytic proton flux. HK1 overexpression reduced tumor burden in an intraocular tumor xenograft model. AMPKa activation by AICAR also enhanced the tumoricidal effects of the chemotherapeutic drug topotecan in vivo. Therefore, enhancing HK1 or AMPKa activity can reprogram cancer metabolism and sensitize Rb tumors to lower doses of existing treatments, a potential therapeutic modality for Rb.

KW - AMPKa

KW - Cancer

KW - Glycolysis

KW - Hexokinase-1

KW - Oxidative phosphorylation

KW - Retinoblastoma

U2 - 10.1016/j.trsl.2023.07.001

DO - 10.1016/j.trsl.2023.07.001

M3 - Article

C2 - 37419277

SN - 1931-5244

VL - 261

SP - 41

EP - 56

JO - Translational Research

JF - Translational Research

IS - 1

ER -