KRAS controls pancreatic cancer cell lipid metabolism and invasive potential through the lipase HSL

Oncogene-induced metabolic reprogramming is a hallmark of pancreatic cancer (PDAC), yet the metabolic drivers of metastasis are unclear. In PDAC, obesity and excess fatty acids accelerate tumor growth and increase metastasis. Here, we report that excess lipids, stored in organelles called lipid droplets (LD), are a key resource to fuel the energy-intensive process of metastasis. The oncogene KRAS…

Read the full article here

Source: Cancer Research
Categories: Hem/Onc News and Journals, Latest Headlines
Tags: ,
Tweets with this article
Cancer Research
Lipid droplets fuel #metastasis in #PancreaticCancer. Lipid storage/utilization are controlled by KRAS-dependent regulation of hormone sensitive lipase and disruption of the KRAS-HSL axis inhibits metastasis. @ginarazidlo https://t.co/IXkOQnj1Qq https://t.co/UeyNWqaZ8X

Related Articles