TY - JOUR
T1 - The catalytic activity of serine hydroxymethyltransferase is essential for de novo nuclear dTMP synthesis in lung cancer cells
AU - Giardina, Giorgio
AU - Paone, Alessio
AU - Tramonti, Angela
AU - Lucchi, Roberta
AU - Marani, Marina
AU - Magnifico, Maria Chiara
AU - Bouzidi, Amani
AU - Pontecorvi, Valentino
AU - Guiducci, Giulia
AU - Zamparelli, Carlotta
AU - Rinaldo, Serena
AU - Paiardini, Alessandro
AU - Contestabile, Roberto
AU - Cutruzzolà, Francesca
N1 - Publisher Copyright:
© 2018 Federation of European Biochemical Societies
PY - 2018/9
Y1 - 2018/9
N2 - Cancer cells reprogramme one-carbon metabolism (OCM) to sustain growth and proliferation. Depending on cell demands, serine hydroxymethyltransferase (SHMT) dynamically changes the fluxes of OCM by reversibly converting serine and tetrahydrofolate (THF) into 5,10-methylene-THF and glycine. SHMT is a tetrameric enzyme that mainly exists in three isoforms; two localize in the cytosol (SHMT1/SHMT2α) and one (SHMT2) in the mitochondria. Both the cytosolic isoforms can also translocate to the nucleus to sustain de novo thymidylate synthesis and support cell proliferation. Finally, the expression levels of the different isoforms are regulated to a certain extent by a yet unknown crosstalk mechanism. We have designed and fully characterized a set of three SHMT1 mutants, which uncouple the oligomeric state of the enzyme from its catalytic activity. We have then investigated the effects of the mutations on SHMT1 nuclear localization, cell viability and crosstalk in lung cancer cells (A549; H1299). Our data reveal that in these cell lines de novo thymidylate synthesis requires SHMT1 to be active, regardless of its oligomeric state. We have also confirmed that the crosstalk between the cytosolic and mitochondrial SHMT actually takes place and regulates the expression of the two isoforms. Apparently, the crosstalk mechanism is independent from the oligomeric state and the catalytic activity of SHMT1. Database: Structural data are available in the PDB under the accession number 6FL5.
AB - Cancer cells reprogramme one-carbon metabolism (OCM) to sustain growth and proliferation. Depending on cell demands, serine hydroxymethyltransferase (SHMT) dynamically changes the fluxes of OCM by reversibly converting serine and tetrahydrofolate (THF) into 5,10-methylene-THF and glycine. SHMT is a tetrameric enzyme that mainly exists in three isoforms; two localize in the cytosol (SHMT1/SHMT2α) and one (SHMT2) in the mitochondria. Both the cytosolic isoforms can also translocate to the nucleus to sustain de novo thymidylate synthesis and support cell proliferation. Finally, the expression levels of the different isoforms are regulated to a certain extent by a yet unknown crosstalk mechanism. We have designed and fully characterized a set of three SHMT1 mutants, which uncouple the oligomeric state of the enzyme from its catalytic activity. We have then investigated the effects of the mutations on SHMT1 nuclear localization, cell viability and crosstalk in lung cancer cells (A549; H1299). Our data reveal that in these cell lines de novo thymidylate synthesis requires SHMT1 to be active, regardless of its oligomeric state. We have also confirmed that the crosstalk between the cytosolic and mitochondrial SHMT actually takes place and regulates the expression of the two isoforms. Apparently, the crosstalk mechanism is independent from the oligomeric state and the catalytic activity of SHMT1. Database: Structural data are available in the PDB under the accession number 6FL5.
KW - lung cancer
KW - OCM
KW - PPI
KW - quaternary structure
KW - SGOCM
KW - tetramer
UR - http://www.scopus.com/inward/record.url?scp=85052452668&partnerID=8YFLogxK
U2 - 10.1111/febs.14610
DO - 10.1111/febs.14610
M3 - Article
C2 - 30035852
AN - SCOPUS:85052452668
SN - 1742-464X
VL - 285
SP - 3238
EP - 3253
JO - FEBS Journal
JF - FEBS Journal
IS - 17
ER -