Lactate, a putative survival factor for myeloma cells, is incorporated by myeloma cells through monocarboxylate transporters 1

Lactate levels within tumors are correlated with metastases, tumor recurrence, and radioresistance, thus apparently contributing to poor outcomes in patients with various cancers. We previously reported that high-level production of lactate by multiple myeloma (MM) cell lines is associated with high...

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Published in:Experimental hematology & oncology 2015-04, Vol.4 (1), p.12-12, Article 12
Main Authors: Fujiwara, Shiho, Wada, Naoko, Kawano, Yawara, Okuno, Yutaka, Kikukawa, Yoshitaka, Endo, Shinya, Nishimura, Nao, Ueno, Nina, Mitsuya, Hiroaki, Hata, Hiroyuki
Format: Article
Language:English
Subjects:
Analysis
Apoptosis
Cancer
Cell cycle
Dehydrogenases
Development and progression
Gene expression
Genetic aspects
Kinases
Lactates
Lymphoma
Medical prognosis
Metastasis
Multiple myeloma
Nitriles
Patient outcomes
Patients
Tumors
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Summary:Lactate levels within tumors are correlated with metastases, tumor recurrence, and radioresistance, thus apparently contributing to poor outcomes in patients with various cancers. We previously reported that high-level production of lactate by multiple myeloma (MM) cell lines is associated with high-level LDH activity within such MM cells. However, the kinetics of lactate remains to be studied. In the present study, we attempted to elucidate the mechanism of lactate incorporation into MM cells. Six MM cell lines and stromal cells obtained through long-term culture of bone marrow samples from MM patients were employed. Incorporation of lactate was quantified using C(14)-labeled lactate. The role of MCT1, a member of the monocarboxylate transporters (MCTs), expressed on MM cells, was examined in the presence of its inhibitor (α-cyano-4-hydroxycinnamic acid: CHC) and by using gene-silencing technique. MM cell lines as well as stromal cells were found to produce lactate. Incorporation of C(14)-labeled lactate into MM cells occurred in all 6 MM cell lines analyzed. Inhibition of MCT1 by using CHC or MCT1-targeting siRNA reduced lactate incorporation and caused apoptosis in MM cells. This apoptosis was enhanced when the activity of pyruvate dehydrogenase kinase was blocked by dichroloacetate. Survival of normal peripheral blood mononuclear cells was not influenced by MCT1 inhibition. The present data suggest that lactate is produced by MM cell lines and stromal cells, and contributes to the survival of such MM cells in autocrine or paracrine manners. Suppression of lactate incorporation by targeting MCT1 may provide a novel therapeutic strategy for MM which may be applicable for other B-cell neoplasms.
ISSN:2162-3619
2162-3619
DOI:10.1186/s40164-015-0008-z