Anne Gemmink1, Sabine Daemen1, Helma J H Kuijpers2, Gert Schaart1, Hans Duimel2, Carmen López-Iglesias2, Marc A M J van Zandvoort3, Kèvin Knoops2, Matthijs K C Hesselink4. 1. Department of Nutrition and Movement Sciences, Maastricht University Medical Centre+, 6200 MD Maastricht, the Netherlands; NUTRIM School for Nutrition and Translational Research in Metabolism, Maastricht, the Netherlands. 2. Microscopy Core Lab, FHML and M4I Maastricht Multimodal Molecular Imaging Institute, Maastricht University, 6200 MD Maastricht, the Netherlands. 3. Department of Genetics & Cell Biology - Molecular Cell Biology, Maastricht University Medical Centre+, 6200 MD Maastricht, the Netherlands; CARIM - Cardiovascular Research Institute Maastricht, Maastricht, the Netherlands; Institute for Molecular Cardiovascular Research IMCAR, Universitätsklinikum, Aachen, Pauwelstrasse 30, Aachen, Germany. 4. Department of Nutrition and Movement Sciences, Maastricht University Medical Centre+, 6200 MD Maastricht, the Netherlands; NUTRIM School for Nutrition and Translational Research in Metabolism, Maastricht, the Netherlands. Electronic address: Matthijs.hesselink@maastrichtuniversity.nl.
Abstract
OBJECTIVE: Intramyocellular lipid droplets (LD) and their coat proteins PLIN2 and PLIN5 are involved in lipolysis, with a putative role for PLIN5 in mitochondrial tethering. Reportedly, these proteins co-localize and cover the surface of the LD. To provide the spatial basis for understanding how these proteins possess their distinct roles, we examined the precise location of PLIN2 and PLIN5 and explored PLIN5 presence at LD-mitochondria contact sites using Stimulated emission depletion (STED) microscopy and correlative light-electron microscopy (CLEM) in human skeletal muscle sections. METHODS: LDs were stained by MDH together with combinations of mitochondrial proteins and PLINs. Subcellular distribution and co-localization of PLIN proteins and mitochondria was imaged by STED microscopy (Leica TCS SP8) and quantified using Pearson's correlation coefficients and intensity profile plots. CLEM was employed to examine the presence of PLIN5 on mitochondria-LD contact sites. RESULTS: Both PLIN2 and PLIN5 localized to the LD in a dot-like, juxtaposed fashion rather than colocalizing and covering the entire LD. Both STED and CLEM revealed a high fraction of PLIN5 at the LD-mitochondria interface, but not at mitochondrial cristae, as suggested previously. CONCLUSION: Using two super-resolution imaging approaches, this is the first study to show that in sections of human skeletal muscle PLIN2 and PLIN5 localize to the LD at distinct sites, with abundance of PLIN5 at LD-mitochondria tethering sites. This novel spatial information uncovers that PLIN proteins do not serve as lipolytic barriers but rather are docking sites for proteins facilitating selective lipase access under a variety of lipolytic conditions.
OBJECTIVE: Intramyocellular lipid droplets (LD) and their coat proteins PLIN2 and PLIN5 are involved in lipolysis, with a putative role for PLIN5 in mitochondrial tethering. Reportedly, these proteins co-localize and cover the surface of the LD. To provide the spatial basis for understanding how these proteins possess their distinct roles, we examined the precise location of PLIN2 and PLIN5 and explored PLIN5 presence at LD-mitochondria contact sites using Stimulated emission depletion (STED) microscopy and correlative light-electron microscopy (CLEM) in human skeletal muscle sections. METHODS: LDs were stained by MDH together with combinations of mitochondrial proteins and PLINs. Subcellular distribution and co-localization of PLIN proteins and mitochondria was imaged by STED microscopy (Leica TCS SP8) and quantified using Pearson's correlation coefficients and intensity profile plots. CLEM was employed to examine the presence of PLIN5 on mitochondria-LD contact sites. RESULTS: Both PLIN2 and PLIN5 localized to the LD in a dot-like, juxtaposed fashion rather than colocalizing and covering the entire LD. Both STED and CLEM revealed a high fraction of PLIN5 at the LD-mitochondria interface, but not at mitochondrial cristae, as suggested previously. CONCLUSION: Using two super-resolution imaging approaches, this is the first study to show that in sections of human skeletal muscle PLIN2 and PLIN5 localize to the LD at distinct sites, with abundance of PLIN5 at LD-mitochondria tethering sites. This novel spatial information uncovers that PLIN proteins do not serve as lipolytic barriers but rather are docking sites for proteins facilitating selective lipase access under a variety of lipolytic conditions.
Authors: Jacob T Seibert; Charles P Najt; Timothy D Heden; Douglas G Mashek; Lisa S Chow Journal: Trends Endocrinol Metab Date: 2020-09-08 Impact factor: 12.015
Authors: Andrea Coppa; Sanjib Guha; Stéphane Fourcade; Janani Parameswaran; Montserrat Ruiz; Ann B Moser; Agatha Schlüter; Michael P Murphy; Jose Miguel Lizcano; Antonio Miranda-Vizuete; Esther Dalfó; Aurora Pujol Journal: Free Radic Biol Med Date: 2020-02-01 Impact factor: 7.376