AI Article Synopsis

  • Researchers are studying how highly curved membrane regions (around 50 nm) affect protein functions in cells, using small, defined liposomes as model membranes.
  • They developed a new sorting technique employing cholesterol-modified DNA 'nanobricks' to classify liposomes by buoyant density, creating consistent populations of sizes between 30-130 nm.
  • This innovative method improves liposome size uniformity and enhances research into how membrane curvature impacts specific protein activities, potentially aiding drug-delivery system development.

Article Abstract

In cells, myriad membrane-interacting proteins generate and maintain curved membrane domains with radii of curvature around or below 50 nm. To understand how such highly curved membranes modulate specific protein functions, and vice versa, it is imperative to use small liposomes with precisely defined attributes as model membranes. Here, we report a versatile and scalable sorting technique that uses cholesterol-modified DNA 'nanobricks' to differentiate hetero-sized liposomes by their buoyant densities. This method separates milligrams of liposomes, regardless of their origins and chemical compositions, into six to eight homogeneous populations with mean diameters of 30-130 nm. We show that these uniform, leak-resistant liposomes serve as ideal substrates to study, with an unprecedented resolution, how membrane curvature influences peripheral (ATG3) and integral (SNARE) membrane protein activities. Compared with conventional methods, our sorting technique represents a streamlined process to achieve superior liposome size uniformity, which benefits research in membrane biology and the development of liposomal drug-delivery systems.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8049973PMC
http://dx.doi.org/10.1038/s41557-021-00667-5DOI Listing

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