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Melanoma brain metastasis is independent of lactate dehydrogenase A expression

Authors :
Rudi Beschorner
Frits Thorsen
Kristine Eldevik Fasmer
Patrick N. Harter
Heidi Espedal
Rolf Bjerkvig
Cecilie Brekke Rygh
Benjamin Weide
Michel Mittelbronn
Erlend Hodneland
Kai Ove Skaftnesmo
Benjamin Bender
Morten Lund-Johansen
Sindre Horn
Terje Sundstrøm
Source :
Neuro-Oncology. 17:1374-1385
Publication Year :
2015
Publisher :
Oxford University Press (OUP), 2015.

Abstract

Background The key metabolic enzyme lactate dehydrogenase A (LDHA) is overexpressed in many cancers, and several preclinical studies have shown encouraging results of targeted inhibition. However, the mechanistic importance of LDHA in melanoma is largely unknown and hitherto unexplored in brain metastasis. Methods We investigated the spatial, temporal, and functional features of LDHA expression in melanoma brain metastasis across multiple in vitro assays, in a robust and predictive animal model employing MRI and PET imaging, and in a unique cohort of 80 operated patients. We further assessed the genomic and proteomic landscapes of LDHA in different cancers, particularly melanomas. Results LDHA expression was especially strong in early and small brain metastases in vivo and related to intratumoral hypoxia in late and large brain metastases in vivo and in patients. However, LDHA expression in human brain metastases was not associated with the number of tumors, BRAF(V600E) status, or survival. Moreover, LDHA depletion by small hairpin RNA interference did not affect cell proliferation or 3D tumorsphere growth in vitro or brain metastasis formation or survival in vivo. Integrated analyses of the genomic and proteomic landscapes of LDHA indicated that LDHA is present but not imperative for tumor progression within the CNS, or predictive of survival in melanoma patients. Conclusions In a large patient cohort and in a robust animal model, we show that although LDHA expression varies biphasically during melanoma brain metastasis formation, tumor progression and survival seem to be functionally independent of LDHA.

Details

ISSN :
15235866 and 15228517
Volume :
17
Database :
OpenAIRE
Journal :
Neuro-Oncology
Accession number :
edsair.doi.dedup.....c5f5232e4c949526001c6c33b68e13f5
Full Text :
https://doi.org/10.1093/neuonc/nov040