Binding of βL-Crystallin with Models of Animal and Human Eye Lens-Lipid Membrane

Preston Hazen; Geraline Trossi-Torres; Nawal K Khadka; Raju Timsina; Laxman Mainali

doi:10.3390/ijms241713600

Binding of β_L-Crystallin with Models of Animal and Human Eye Lens-Lipid Membrane

Int J Mol Sci. 2023 Sep 2;24(17):13600. doi: 10.3390/ijms241713600.

Authors

Preston Hazen¹, Geraline Trossi-Torres^{1

2}, Nawal K Khadka², Raju Timsina², Laxman Mainali^{1

2}

Affiliations

¹ Biomolecular Sciences Graduate Programs, Boise State University, Boise, ID 83725, USA.
² Department of Physics, Boise State University, Boise, ID 83725, USA.

Abstract

Several discoveries show that with age and cataract formation, β-crystallin binds with the lens membrane or associates with other lens proteins, which bind with the fiber cell plasma membrane, accompanied by light scattering and cataract formation. However, how lipids (phospholipids and sphingolipids) and cholesterol (Chol) influence β-crystallin binding to the membrane is unclear. This research aims to elucidate the role of lipids and Chol in the binding of β-crystallin to the membrane and the membrane's physical properties (mobility, order, and hydrophobicity) with β-crystallin binding. We used electron paramagnetic resonance (EPR) spin-labeling methods to investigate the binding of β_L-crystallin with a model of porcine lens-lipid (MPLL), model of mouse lens-lipid (MMLL), and model of human lens-lipid (MHLL) membrane with and without Chol. Our results show that β_L-crystallin binds with all of the investigated membranes in a saturation manner, and the maximum parentage of the membrane surface occupied (MMSO) by β_L-crystallin and the binding affinity (K_a) of β_L-crystallin to the membranes followed trends: MMSO (MPLL) > MMSO (MMLL) > MMSO (MHLL) and K_a (MHLL) > K_a (MMLL) ≈ K_a (MPLL), respectively, in which the presence of Chol reduces the MMSO and K_a for all membranes. The mobility near the headgroup regions of the membranes decreases with an increase in the binding of β_L-crystallin; however, the decrease is more pronounced in the MPLL and MMLL membranes than the MHLL membrane. In the MPLL and MMLL membranes, the membranes become slightly ordered near the headgroup with an increase in β_L-crystallin binding compared to the MHLL membrane. The hydrophobicity near the headgroup region of the membrane increases with β_L-crystallin binding; however, the increase is more pronounced in the MPLL and MMLL membranes than the MHLL membrane, indicating that β_L-crystallin binding creates a hydrophobic barrier for the passage of polar molecules, which supports the barrier hypothesis in cataract formation. However, in the presence of Chol, there is no significant increase in hydrophobicity with β_L-crystallin binding, suggesting that Chol prevents the formation of a hydrophobic barrier, possibly protecting against cataract formation.

Keywords: EPR spin-labeling method; binding affinity (Ka); cataracts; cholesterol; cholesterol bilayer domains; hydrophobicity; maximum percentage of membrane surface occupied (MMSO); maximum splitting; mobility parameter; percentage of membrane surface occupied (MSO); βL-crystallin.

MeSH terms

Animals
Cataract*
Crystallins*
Humans
Lens, Crystalline*
Mice
Phospholipids
Swine
beta-Crystallins

Substances

Crystallins
beta-Crystallins
Phospholipids

Abstract

MeSH terms

Substances

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