Lipid-bound ApoE3 self-assemble into elliptical disc-shaped particles
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Lipid-bound ApoE3 self-assemble into elliptical disc-shaped particles. / Larsen, Andreas Haahr; Johansen, Nicolai Tidemand; Gajhede, Michael; Arleth, Lise; Midtgaard, Soren Roi.
In: B B A - Biomembranes, Vol. 1863, No. 1, 183495, 2021.Research output: Contribution to journal › Journal article › peer-review
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TY - JOUR
T1 - Lipid-bound ApoE3 self-assemble into elliptical disc-shaped particles
AU - Larsen, Andreas Haahr
AU - Johansen, Nicolai Tidemand
AU - Gajhede, Michael
AU - Arleth, Lise
AU - Midtgaard, Soren Roi
PY - 2021
Y1 - 2021
N2 - Apolipoproteins are vital to lipid metabolism and cholesterol transport in the human body. Here we present a structural study of the lipid-bound particles formed by ApoE3 in a full-length and a truncated version. The particles are formed with, respectively, POPC and DMPC and investigated by small-angle X-ray scattering and negative stain electron microscopy. We find that lipid-bound ApoE3 particles are elliptical, disc-shaped particles composed of a central lipid bilayer encircled by two amphipathic ApoE3 proteins. We went on to investigate a truncated form of ApoE3 containing only residue 80 to 255 (ApoE380-255), which is the central helical repeat segment of ApoE3. The lipid-bound ApoE380-255 particles are found to have the same morphology as the particles with full-length ApoE3. However, they are larger, and form more heterogeneous discoidal structures with four proteins per particle. This behavior is in contrast to ApoA1 where the highly similar helical repeat domain determines the size and stoichiometry of the formed particles both in the case of full-length and truncated ApoA1. Our data hence points towards different mechanisms for lipid bilayer structural modulation by ApoA1 and ApoE3 due to different roles of the non-repeat segments.
AB - Apolipoproteins are vital to lipid metabolism and cholesterol transport in the human body. Here we present a structural study of the lipid-bound particles formed by ApoE3 in a full-length and a truncated version. The particles are formed with, respectively, POPC and DMPC and investigated by small-angle X-ray scattering and negative stain electron microscopy. We find that lipid-bound ApoE3 particles are elliptical, disc-shaped particles composed of a central lipid bilayer encircled by two amphipathic ApoE3 proteins. We went on to investigate a truncated form of ApoE3 containing only residue 80 to 255 (ApoE380-255), which is the central helical repeat segment of ApoE3. The lipid-bound ApoE380-255 particles are found to have the same morphology as the particles with full-length ApoE3. However, they are larger, and form more heterogeneous discoidal structures with four proteins per particle. This behavior is in contrast to ApoA1 where the highly similar helical repeat domain determines the size and stoichiometry of the formed particles both in the case of full-length and truncated ApoA1. Our data hence points towards different mechanisms for lipid bilayer structural modulation by ApoA1 and ApoE3 due to different roles of the non-repeat segments.
KW - Small-angle X-ray scattering, SAXS
KW - High density lipoprotein, HDL
KW - Nanodisc
KW - Apolipoprotein E, ApoE
KW - Lipoprotein
KW - Electron microscopy, EM
KW - HIGH-DENSITY-LIPOPROTEIN
KW - NEGATIVE-STAINING PROTOCOL
KW - HUMAN APOLIPOPROTEIN E3
KW - X-RAY-SCATTERING
KW - NEUTRON-SCATTERING
KW - MEMBRANE-PROTEINS
KW - A-I
KW - CHOLESTEROL
KW - NANODISCS
KW - MODEL
U2 - 10.1016/j.bbamem.2020.183495
DO - 10.1016/j.bbamem.2020.183495
M3 - Journal article
C2 - 33189719
VL - 1863
JO - B B A - Biomembranes
JF - B B A - Biomembranes
SN - 0005-2736
IS - 1
M1 - 183495
ER -
ID: 255730599