Characterization of cancer-related somatic mutations in the adenosine A2B receptor

Xuesong Wang; Willem Jespers; Brandon J Bongers; Maria C C Habben Jansen; Chantal M Stangenberger; Majlen A Dilweg; Hugo Gutiérrez-de-Terán; Adriaan P IJzerman; Laura H Heitman; Gerard J P van Westen

doi:10.1016/j.ejphar.2020.173126

Characterization of cancer-related somatic mutations in the adenosine A_2B receptor

Eur J Pharmacol. 2020 Aug 5:880:173126. doi: 10.1016/j.ejphar.2020.173126. Epub 2020 Apr 26.

Affiliations

¹ Drug Discovery and Safety, Leiden Academic Centre for Drug Research, Einsteinweg 55, 2333 CC, Leiden, the Netherlands.
² Drug Discovery and Safety, Leiden Academic Centre for Drug Research, Einsteinweg 55, 2333 CC, Leiden, the Netherlands; Department of Cell and Molecular Biology, Uppsala University, Biomedical Center, Box 596, SE-751 24, Uppsala, Sweden.
³ Department of Cell and Molecular Biology, Uppsala University, Biomedical Center, Box 596, SE-751 24, Uppsala, Sweden.
⁴ Drug Discovery and Safety, Leiden Academic Centre for Drug Research, Einsteinweg 55, 2333 CC, Leiden, the Netherlands. Electronic address: l.h.heitman@lacdr.leidenuniv.nl.
⁵ Drug Discovery and Safety, Leiden Academic Centre for Drug Research, Einsteinweg 55, 2333 CC, Leiden, the Netherlands. Electronic address: gerard@lacdr.leidenuniv.nl.

PMID: 32348778
DOI: 10.1016/j.ejphar.2020.173126

Abstract

In cancer, G protein-coupled receptors (GPCRs) are involved in tumor progression and metastasis. In this study we particularly examined one GPCR, the adenosine A_2B receptor. This receptor is activated by high concentrations of its endogenous ligand adenosine, which suppresses the immune response to fight tumor progression. A series of adenosine A_2B receptor mutations were retrieved from the Cancer Genome Atlas harboring data from patient samples with different cancer types. The main goal of this work was to investigate the pharmacology of these mutant receptors using a 'single-GPCR-one-G protein' yeast assay technology. Concentration-growth curves were obtained with the full agonist NECA for the wild-type receptor and 15 mutants. Compared to wild-type receptor, the constitutive activity levels in mutant receptors F141L^4.61, Y202C^5.58 and L310P^8.63 were high, while the potency and efficacy of NECA and BAY 60-6583 on Y202C^5.58 was lower. A 33- and 26-fold higher constitutive activity on F141L^4.61 and L310P^8.63 was reduced to wild-type levels in response to the inverse agonist ZM241385. These constitutively active mutants may thus be tumor promoting. Mutant receptors F259S^6.60 and Y113F^34.53 showed a more than one log-unit decrease in potency. A complete loss of activation was observed in mutant receptors C29R^1.54, W130C^4.50 and P249L^6.50. All mutations were characterized at the structural level, generating hypotheses of their roles on modulating the receptor conformational equilibrium. Taken together, this study is the first to investigate the nature of adenosine A_2B receptor cancer mutations and may thus provide insights in mutant receptor function in cancer.

Keywords: Cancer-related mutations; G protein-coupled receptor; Yeast system.

MeSH terms

Adenosine A2 Receptor Agonists / pharmacology
Adenosine-5'-(N-ethylcarboxamide) / pharmacology
Aminopyridines / pharmacology
Computational Biology
Humans
Models, Molecular
Mutation
Neoplasms / genetics*
Receptor, Adenosine A2B / genetics*
Receptor, Adenosine A2B / metabolism
Saccharomyces cerevisiae / genetics

Substances

Adenosine A2 Receptor Agonists
Aminopyridines
BAY 60-6583
Receptor, Adenosine A2B
Adenosine-5'-(N-ethylcarboxamide)