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Suppression of pyruvate dehydrogenase kinase by dichloroacetate in cancer and skeletal muscle cells is isoform specific and partially independent of HIF-1α
ID
Škorja, Nives
(
Author
),
ID
Dolinar, Klemen
(
Author
),
ID
Miš, Katarina
(
Author
),
ID
Matkovič, Urška
(
Author
),
ID
Bizjak, Maruša
(
Author
),
ID
Pavlin, Mojca
(
Author
),
ID
Podbregar, Matej
(
Author
),
ID
Pirkmajer, Sergej
(
Author
)
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https://www.mdpi.com/1422-0067/22/16/8610
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Abstract
Inhibition of pyruvate dehydrogenase kinase (PDK) emerged as a potential strategy for treatment of cancer and metabolic disorders. Dichloroacetate (DCA), a prototypical PDK inhibitor, reduces the abundance of some PDK isoenzymes. However, the underlying mechanisms are not fully characterized and may differ across cell types. We determined that DCA reduced the abundance of PDK1 in breast (MDA-MB-231) and prostate (PC-3) cancer cells, while it suppressed both PDK1 and PDK2 in skeletal muscle cells (L6 myotubes). The DCA-induced PDK1 suppression was partially dependent on hypoxia-inducible factor-1α (HIF-1α), a transcriptional regulator of PDK1, in cancer cells but not in L6 myotubes. However, the DCA-induced alterations in the mRNA and the protein levels of PDK1 and/or PDK2 did not always occur in parallel, implicating a role for post-transcriptional mechanisms. DCA did not inhibit the mTOR signaling, while inhibitors of the proteasome or gene silencing of mitochondrial proteases CLPP and AFG3L2 did not prevent the DCA-induced reduction of the PDK1 protein levels. Collectively, our results suggest that DCA reduces the abundance of PDK in an isoform-dependent manner via transcriptional and post-transcriptional mechanisms. Differential response of PDK isoenzymes to DCA might be important for its pharmacological effects in different types of cells.
Language:
English
Keywords:
skeletal muscle cells
,
cancer
,
dichloroacetate
,
pyruvate dehydrogenase kinase
,
pyruvate dehydrogenase complex
,
myotubes
Work type:
Article
Typology:
1.01 - Original Scientific Article
Organization:
MF - Faculty of Medicine
FE - Faculty of Electrical Engineering
FFA - Faculty of Pharmacy
Publication status:
Published
Publication version:
Version of Record
Year:
2021
Number of pages:
26 str.
Numbering:
Vol. 22, iss. 16, art. 8610
PID:
20.500.12556/RUL-135749
UDC:
616-006
ISSN on article:
1422-0067
DOI:
10.3390/ijms22168610
COBISS.SI-ID:
72730115
Publication date in RUL:
30.03.2022
Views:
964
Downloads:
246
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Record is a part of a journal
Title:
International journal of molecular sciences
Shortened title:
Int. j. mol. sci.
Publisher:
MDPI
ISSN:
1422-0067
COBISS.SI-ID:
2779162
Licences
License:
CC BY 4.0, Creative Commons Attribution 4.0 International
Link:
http://creativecommons.org/licenses/by/4.0/
Description:
This is the standard Creative Commons license that gives others maximum freedom to do what they want with the work as long as they credit the author.
Licensing start date:
10.08.2021
Secondary language
Language:
Slovenian
Keywords:
celice skeletnih mišic
,
rak
,
dikloroacetat
Projects
Funder:
ARRS - Slovenian Research Agency
Project number:
P3-0043
Name:
Molekularni mehanizmi razvoja in delovanja skeletne mišice
Funder:
ARRS - Slovenian Research Agency
Project number:
J7-8276
Name:
Vpliv protirevmatičnih zdravil na inzulinsko rezistenco in energijsko presnovo v skeletni mišici
Funder:
ARRS - Slovenian Research Agency
Project number:
J3-6794
Name:
Celična energijska presnova kot tarča za zdravljenje raka – genski in farmakološki pristop
Funder:
ARRS - Slovenian Research Agency
Project number:
J3-2523
Name:
Disregulacija presnove v astrogliji pri nevrodegeneraciji
Funder:
ARRS - Slovenian Research Agency
Project number:
P1-0055
Name:
Biofizika polimerov, membran, gelov, koloidov in celic
Funder:
ARRS - Slovenian Research Agency
Funding programme:
Young researchers
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