AI Article Synopsis

  • Lung cancer is the top cause of cancer deaths, particularly affecting those with squamous cell carcinoma (SCC), where few treatment options exist beyond the initial therapy.
  • Researchers studied the phospholipid profiles of 30 human SCCs and found that nearly all samples had longer acyl chains in their phospholipids compared to normal tissues, a change confirmed in both human samples and mouse models.
  • The study identified ELOVL6 as the key enzyme responsible for this acyl chain elongation, and inhibiting it significantly hindered the growth of SCC cells, suggesting ELOVL6 could be a new target for lung cancer treatment.

Article Abstract

Lung cancer is the leading cause of cancer death. Beyond first line treatment, few therapeutic options are available, particularly for squamous cell carcinoma (SCC). Here, we have explored the phospholipidomes of 30 human SCCs and found that they almost invariably (in 96.7% of cases) contain phospholipids with longer acyl chains compared to matched normal tissues. This trait was confirmed using in situ 2D-imaging MS on tissue sections and by phospholipidomics of tumor and normal lung tissue of the L-IkkαKA/KA mouse model of lung SCC. In both human and mouse, the increase in acyl chain length in cancer tissue was accompanied by significant changes in the expression of acyl chain elongases (ELOVLs). Functional screening of differentially expressed ELOVLs by selective gene knockdown in SCC cell lines followed by phospholipidomics revealed ELOVL6 as the main elongation enzyme responsible for acyl chain elongation in cancer cells. Interestingly, inhibition of ELOVL6 drastically reduced colony formation of multiple SCC cell lines in vitro and significantly attenuated their growth as xenografts in vivo in mouse models. These findings identify acyl chain elongation as one of the most common traits of lung SCC discovered so far and pinpoint ELOVL6 as a novel potential target for cancer intervention.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4914306PMC
http://dx.doi.org/10.18632/oncotarget.7179DOI Listing

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