Literature DB >> 36120532

Quantitative Models of Lipid Transfer and Membrane Contact Formation.

Yongli Zhang1,2, Jinghua Ge1, Xin Bian1,3,4, Avinash Kumar1.   

Abstract

Lipid transfer proteins (LTPs) transfer lipids between different organelles, and thus play key roles in lipid homeostasis and organelle dynamics. The lipid transfer often occurs at the membrane contact sites (MCS) where two membranes are held within 10-30 nm. While most LTPs act as a shuttle to transfer lipids, recent experiments reveal a new category of eukaryotic LTPs that may serve as a bridge to transport lipids in bulk at MCSs. However, the molecular mechanisms underlying lipid transfer and MCS formation are not well understood. Here, we first review two recent studies of extended synaptotagmin (E-Syt)-mediated membrane binding and lipid transfer using novel approaches. Then we describe mathematical models to quantify the kinetics of lipid transfer by shuttle LTPs based on a lipid exchange mechanism. We find that simple lipid mixing among membranes of similar composition and/or lipid partitioning among membranes of distinct composition can explain lipid transfer against a concentration gradient widely observed for LTPs. We predict that selective transport of lipids, but not membrane proteins, by bridge LTPs leads to osmotic membrane tension by analogy to the osmotic pressure across a semipermeable membrane. A gradient of such tension and the conventional membrane tension may drive bulk lipid flow through bridge LTPs at a speed consistent with the fast membrane expansion observed in vivo. Finally, we discuss the implications of membrane tension and lipid transfer in organelle biogenesis. Overall, the quantitative models may help clarify the mechanisms of LTP-mediated MCS formation and lipid transfer.

Entities:  

Keywords:  ATG2; DNA origami; Lipid transfer protein (LTP); VPS13; extended synaptotagmin (E-Syt); lipid exchange; membrane contact site (MCS); optical tweezers; osmotic membrane tension

Year:  2022        PMID: 36120532      PMCID: PMC9481209          DOI: 10.1177/25152564221096024

Source DB:  PubMed          Journal:  Contact (Thousand Oaks)        ISSN: 2515-2564


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