AI Article Synopsis
- Cachexia is a severe energy-wasting syndrome commonly seen in cancer patients, leading to significant muscle and fat loss.
- Tumor exposure in mice initiated a cycle of energy loss in fat cells, marked by both fat breakdown and creation, alongside inactivated AMP-activated protein kinase (Ampk), which usually helps maintain energy levels.
- The introduction of an Ampk-stabilizing peptide (ACIP) showed promise in reducing fat wasting, suggesting that maintaining Ampk function could be a potential therapeutic approach for cachexia.
Article Abstract
Cachexia represents a fatal energy-wasting syndrome in a large number of patients with cancer that mostly results in a pathological loss of skeletal muscle and adipose tissue. Here we show that tumor cell exposure and tumor growth in mice triggered a futile energy-wasting cycle in cultured white adipocytes and white adipose tissue (WAT), respectively. Although uncoupling protein 1 (Ucp1)-dependent thermogenesis was dispensable for tumor-induced body wasting, WAT from cachectic mice and tumor-cell-supernatant-treated adipocytes were consistently characterized by the simultaneous induction of both lipolytic and lipogenic pathways. Paradoxically, this was accompanied by an inactivated AMP-activated protein kinase (Ampk), which is normally activated in peripheral tissues during states of low cellular energy. Ampk inactivation correlated with its degradation and with upregulation of the Ampk-interacting protein Cidea. Therefore, we developed an Ampk-stabilizing peptide, ACIP, which was able to ameliorate WAT wasting in vitro and in vivo by shielding the Cidea-targeted interaction surface on Ampk. Thus, our data establish the Ucp1-independent remodeling of adipocyte lipid homeostasis as a key event in tumor-induced WAT wasting, and we propose the ACIP-dependent preservation of Ampk integrity in the WAT as a concept in future therapies for cachexia.
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| http://dx.doi.org/10.1038/nm.4171 | DOI Listing |
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