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Interfacial binding and aggregation of lamin A tail domains associated with Hutchinson-Gilford progeria syndrome.


ABSTRACT: Hutchinson-Gilford progeria syndrome is a premature aging disorder associated with the expression of ?50 lamin A (?50LA), a mutant form of the nuclear structural protein lamin A (LA). ?50LA is missing 50 amino acids from the tail domain and retains a C-terminal farnesyl group that is cleaved from the wild-type LA. Many of the cellular pathologies of HGPS are thought to be a consequence of protein-membrane association mediated by the retained farnesyl group. To better characterize the protein-membrane interface, we quantified binding of purified recombinant ?50LA tail domain (?50LA-TD) to tethered bilayer membranes composed of phosphatidylserine and phosphocholine using surface plasmon resonance. Farnesylated ?50LA-TD binds to the membrane interface only in the presence of Ca(2+) or Mg(2+) at physiological ionic strength. At extremely low ionic strength, both the farnesylated and non-farnesylated forms of ?50LA-TD bind to the membrane surface in amounts that exceed those expected for a densely packed protein monolayer. Interestingly, the wild-type LA-TD with no farnesylation also associates with membranes at low ionic strength but forms only a single layer. We suggest that electrostatic interactions are mediated by charge clusters with a net positive charge that we calculate on the surface of the LA-TDs. These studies suggest that the accumulation of ?50LA at the inner nuclear membrane observed in cells is due to a combination of aggregation and membrane association rather than simple membrane binding; electrostatics plays an important role in mediating this association.

SUBMITTER: Kalinowski A 

PROVIDER: S-EPMC4212650 | biostudies-literature | 2014 Dec

REPOSITORIES: biostudies-literature

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