POMC Neuron BBSome Regulation of Body Weight is Independent of its Ciliary Function.
Deng-Fu GuoPaul A WilliamsConnor LauleCharles SeabyQihong ZhangVal C SheffieldKamal RahmouniPublished in: Function (Oxford, England) (2023)
The BBSome, a complex of several Bardet-Biedl syndrome (BBS) proteins including BBS1, has emerged as a critical regulator of energy homeostasis. Although the BBSome is best known for its involvement in cilia trafficking, through a process that involve BBS3, it also regulates the localization of cell membrane receptors underlying metabolic regulation. Here, we show that inducible Bbs1 gene deletion selectively in proopiomelanocortin (POMC) neurons cause a gradual increase in body weight, which was associated with higher fat mass. In contrast, inducible deletion of Bbs3 gene in POMC neurons failed to affect body weight and adiposity. Interestingly, loss of BBS1 in POMC neurons led to glucose intolerance and insulin insensitivity, whereas BBS3 deficiency in these neurons is associated with slight impairment in glucose handling, but normal insulin sensitivity. BBS1 deficiency altered the plasma membrane localization of serotonin 5-HT2C receptor (5-HT 2C R) and ciliary trafficking of neuropeptide Y2 receptor (NPY 2 R).In contrast, BBS3 deficiency, which disrupted the ciliary localization of the BBSome, did not interfere with plasma membrane expression of 5-HT 2C R, but reduced the trafficking of NPY 2 R to cilia. We also show that deficiency in BBS1, but not BBS3, alters mitochondria dynamics and decreased total and phosphorylated levels of dynamin-like protein 1 (DRP1) protein. Importantly, rescuing DRP1 activity restored mitochondria dynamics and localization of 5-HT 2C R and NPY 2 R in BBS1-deficient cells. The contrasting effects on energy and glucose homeostasis evoked by POMC neuron deletion of BBS1 versus BBS3 indicate that BBSome regulation of metabolism is not related to its ciliary function in these neurons.
Keyphrases
- body weight
- spinal cord
- type diabetes
- adipose tissue
- poor prognosis
- cell death
- computed tomography
- gene expression
- metabolic syndrome
- skeletal muscle
- induced apoptosis
- blood glucose
- body mass index
- magnetic resonance imaging
- cell proliferation
- replacement therapy
- case report
- signaling pathway
- fatty acid
- endoplasmic reticulum
- long non coding rna
- functional connectivity
- drug induced