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Mitochondrial metabolism in primary and metastatic human kidney cancers.
Bezwada, Divya; Lesner, Nicholas P; Brooks, Bailey; Vu, Hieu S; Wu, Zheng; Cai, Ling; Kasitinon, Stacy; Kelekar, Sherwin; Cai, Feng; Aurora, Arin B; Patrick, McKenzie; Leach, Ashley; Ghandour, Rashed; Zhang, Yuanyuan; Do, Duyen; Sudderth, Jessica; Dumesnil, Dennis; House, Sara; Rosales, Tracy; Poole, Alan M; Lotan, Yair; Woldu, Solomon; Bagrodia, Aditya; Meng, Xiaosong; Cadeddu, Jeffrey A; Mishra, Prashant; Pedrosa, Ivan; Kapur, Payal; Courtney, Kevin D; Malloy, Craig R; Margulis, Vitaly; DeBerardinis, Ralph J.
Afiliação
  • Bezwada D; Children's Medical Center Research Institute.
  • Lesner NP; Children's Medical Center Research Institute.
  • Brooks B; Children's Medical Center Research Institute.
  • Vu HS; Children's Medical Center Research Institute.
  • Wu Z; Children's Medical Center Research Institute.
  • Cai L; Children's Medical Center Research Institute.
  • Kasitinon S; Quantitative Biomedical Research Center.
  • Kelekar S; Children's Medical Center Research Institute.
  • Cai F; Children's Medical Center Research Institute.
  • Aurora AB; Children's Medical Center Research Institute.
  • Patrick M; Children's Medical Center Research Institute.
  • Leach A; Children's Medical Center Research Institute.
  • Ghandour R; Children's Medical Center Research Institute.
  • Zhang Y; Department of Urology.
  • Do D; Children's Medical Center Research Institute.
  • Sudderth J; Children's Medical Center Research Institute.
  • Dumesnil D; Children's Medical Center Research Institute.
  • House S; Children's Medical Center Research Institute.
  • Rosales T; Children's Medical Center Research Institute.
  • Poole AM; Children's Medical Center Research Institute.
  • Lotan Y; Children's Medical Center Research Institute.
  • Woldu S; Department of Pediatrics.
  • Bagrodia A; Department of Urology.
  • Meng X; Department of Urology.
  • Cadeddu JA; Department of Urology.
  • Mishra P; Department of Urology.
  • Pedrosa I; Department of Urology.
  • Kapur P; Children's Medical Center Research Institute.
  • Courtney KD; Department of Pediatrics.
  • Malloy CR; Department of Urology.
  • Margulis V; Department of Radiology.
  • DeBerardinis RJ; Kidney Cancer Program.
bioRxiv ; 2023 Feb 07.
Article em En | MEDLINE | ID: mdl-36798172
ABSTRACT
Most kidney cancers display evidence of metabolic dysfunction1-4 but how this relates to cancer progression in humans is unknown. We used a multidisciplinary approach to infuse 13C-labeled nutrients during surgical tumour resection in over 70 patients with kidney cancer. Labeling from [U-13C]glucose varies across cancer subtypes, indicating that the kidney environment alone cannot account for all metabolic reprogramming in these tumours. Compared to the adjacent kidney, clear cell renal cell carcinomas (ccRCC) display suppressed labelling of tricarboxylic acid (TCA) cycle intermediates in vivo and in organotypic slices cultured ex vivo, indicating that suppressed labeling is tissue intrinsic. Infusions of [1,2-13C]acetate and [U-13C]glutamine in patients, coupled with respiratory flux of mitochondria isolated from kidney and tumour tissue, reveal primary defects in mitochondrial function in human ccRCC. However, ccRCC metastases unexpectedly have enhanced labeling of TCA cycle intermediates compared to primary ccRCCs, indicating a divergent metabolic program during ccRCC metastasis in patients. In mice, stimulating respiration in ccRCC cells is sufficient to promote metastatic colonization. Altogether, these findings indicate that metabolic properties evolve during human kidney cancer progression, and suggest that mitochondrial respiration may be limiting for ccRCC metastasis but not for ccRCC growth at the site of origin.

Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Idioma: En Revista: BioRxiv Ano de publicação: 2023 Tipo de documento: Article

Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Idioma: En Revista: BioRxiv Ano de publicação: 2023 Tipo de documento: Article