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Structure insights of the human peroxisomal ABC transporter ALDP
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AbstractAdrenoleukodystrophy protein (ALDP) is responsible for the transport of free very-long-chain fatty acids (VLCFAs) and corresponding CoA-esters across the peroxisomal membrane. ALDP belongs to the ATP-binding cassette sub-family D, which is also named as ABCD1. Dysfunction of ALDP leads to peroxisomal metabolic disorder exemplified by X-linked adrenoleukodystrophy (ALD). Hundreds of ALD-causing mutations are identified on ALDP. However, the pathogenic mechanisms of these mutations are restricted to clinical description due to limited structural information. Furthermore, ALDP plays a role in myelin maintenance, which is tightly associated with axon regeneration. Here we report the cryo-electron microscopy (cryo-EM) structure of human ALDP with nominal resolution of 3.4 Å in nucleotide free state. The structure of ALDP exhibits a typical assembly of ABC transporters. The nucleotide binding domains (NBDs) displays a ligand free state. ALDP exhibits an inward-open conformation to the cytosol. A short helix is located at the peroxisomal side, which is different from other three members of ABCD transporters. The two transmembrane domains (TMDs) of ALDP form a cavity, in which two lipid-like densities can be recognized as the head group of an coenzyme-A ester of a lipid. This structure provides a framework for understanding the working mechanism of ALDP and classification of the disease-causing mutations.
Title: Structure insights of the human peroxisomal ABC transporter ALDP
Description:
AbstractAdrenoleukodystrophy protein (ALDP) is responsible for the transport of free very-long-chain fatty acids (VLCFAs) and corresponding CoA-esters across the peroxisomal membrane.
ALDP belongs to the ATP-binding cassette sub-family D, which is also named as ABCD1.
Dysfunction of ALDP leads to peroxisomal metabolic disorder exemplified by X-linked adrenoleukodystrophy (ALD).
Hundreds of ALD-causing mutations are identified on ALDP.
However, the pathogenic mechanisms of these mutations are restricted to clinical description due to limited structural information.
Furthermore, ALDP plays a role in myelin maintenance, which is tightly associated with axon regeneration.
Here we report the cryo-electron microscopy (cryo-EM) structure of human ALDP with nominal resolution of 3.
4 Å in nucleotide free state.
The structure of ALDP exhibits a typical assembly of ABC transporters.
The nucleotide binding domains (NBDs) displays a ligand free state.
ALDP exhibits an inward-open conformation to the cytosol.
A short helix is located at the peroxisomal side, which is different from other three members of ABCD transporters.
The two transmembrane domains (TMDs) of ALDP form a cavity, in which two lipid-like densities can be recognized as the head group of an coenzyme-A ester of a lipid.
This structure provides a framework for understanding the working mechanism of ALDP and classification of the disease-causing mutations.
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