Functional Dissection of an AP-2 β2 Appendage-binding Sequence within the Autosomal Recessive Hypercholesterolemia Protein

Mishra, Sanjay; Keyel, Peter A.; Edeling, Melissa A.; Dupin, Amie L.; Owen, David J.; Traub, Linton M.

doi:10.1074/jbc.m501029200

Cited by 58 publications

(78 citation statements)

References 58 publications

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“…Previously identified AP-2 interaction motifs range from small tripeptide (DPF/W) sequences (17) to as many as 16 residues found in ARH or arrestins (29). None of the previously characterized motifs are present in the regions flanking the BRAG2 clathrin boxes, and it is therefore likely that other, unidentified motifs mediate interactions with AP-2.…”

Section: Discussionmentioning

confidence: 99%

BRAG2/GEP100/IQSec1 Interacts with Clathrin and Regulates α5β1 Integrin Endocytosis through Activation of ADP Ribosylation Factor 5 (Arf5)

Moravec

Conger

D’Souza

et al. 2012

Journal of Biological Chemistry

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Background:We previously showed that BRAG2, a known activator of Arf6, regulates cell surface levels of ␤1 integrin. Results: BRAG2 can also activate Arf4 and Arf5, but it is Arf5 that regulates integrin endocytosis. Conclusion: BRAG2 interacts with clathrin and activates Arf5 to enhance integrin internalization. Significance: This is the first evidence of a role for Arf5 at the plasma membrane in the regulation of endocytosis.

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Section: Discussionmentioning

confidence: 99%

BRAG2/GEP100/IQSec1 Interacts with Clathrin and Regulates α5β1 Integrin Endocytosis through Activation of ADP Ribosylation Factor 5 (Arf5)

Moravec

Conger

D’Souza

et al. 2012

Journal of Biological Chemistry

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“…Together, this set of interactions enables ARH to function as an endocytic adaptor for the clathrin-mediated endocytosis of LDLR in the liver. Accordingly, ARH has been classified as a clathrin-associated sorting protein (CLASP) (12), a group of proteins that serve as a molecular bridge between receptors and the clathrin machinery for their endocytic internalization.…”

mentioning

confidence: 99%

Atomic structure of the autosomal recessive hypercholesterolemia phosphotyrosine-binding domain in complex with the LDL-receptor tail

Dvir

Shah

Gottardi

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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Hypercholesterolemia, high serum cholesterol in the form of LDL, is a major risk factor for atherosclerosis. LDL is mostly degraded in the liver after its cellular internalization with the LDL receptor (LDLR). This clathrin-mediated endocytosis depends on the protein autosomal recessive hypercholesterolemia (ARH), which binds the LDLR cytoplasmic tail. Mutations in either the LDLR tail or in ARH lead to hypercholesterolemia and premature atherosclerosis. Despite the significance of this interaction for cholesterol homeostasis, no structure of either ARH or the LDLR tail is available to determine its molecular basis. We report the crystal structure at 1.37-Å resolution of the phosphotyrosine-binding (PTB) domain of ARH in complex with an LDLR tail peptide containing the FxNPxY 0 internalization signal. Surprisingly, ARH interacts with a longer portion of the tail than previously recognized, which extends to I -7 xF -5 xNPxY 0 QK +2 . The LDLR tail assumes a unique "Hook"-like structure with a double β-turn conformation, which is accommodated in distinctive ARH structural determinants (i.e., an extended backbone hydrogen-bonding platform, three hydrophobic helical grooves, and a hydrophobic pocket for Y 0 ). This unique complementarity differs significantly in related PTB proteins and may account for the unique physiological role of these partners in the hepatic uptake of cholesterol LDL. Moreover, the unusual hydrophobic pocket for Y 0 explains the distinctive ability of ARH to internalize proteins containing either FxNPxY 0 or FxNPxF 0 sequences. Biophysical measurements reveal how mutations associated with hypercholesterolemia destabilize ARH and its complex with LDLR and illuminate LDL internalization defects seen in patients.lipoprotein | crystallography | trafficking | lipid metabolism

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“…The former is a transmembrane protein and the second a mannosidase. The latter encodes for a cytosolic protein that interacts with the LDL receptor, and mutations in it have cause hypercholesterolemia, an autosomal recessive disorder (Mishra et al 2005;Quagliarini et al 2007). Negative Tajima's D values $ À2 were found in windows containing HIST2H*, FCGR1A, and PPIAL4, a histone cluster, a fragment of the IgG receptor, and the peptidylprolyl isomerase A, respectively.…”

Section: Resultsmentioning

confidence: 99%

Correcting Estimators of θ and Tajima's D for Ascertainment Biases Caused by the Single-Nucleotide Polymorphism Discovery Process

Ramírez-Soriano

Nielsen

2009

Genetics

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Most single-nucleotide polymorphism (SNP) data suffer from an ascertainment bias caused by the process of SNP discovery followed by SNP genotyping. The final genotyped data are biased toward an excess of common alleles compared to directly sequenced data, making standard genetic methods of analysis inapplicable to this type of data. We here derive corrected estimators of the fundamental population genetic parameter u ¼ 4N e m (N e , effective population size; m, mutation rate) on the basis of the average number of pairwise differences and on the basis of the number of segregating sites. We also derive the variances and covariances of these estimators and provide a corrected version of Tajima's D statistic. We reanalyze a human genomewide SNP data set and find substantial differences in the results with or without ascertainment bias correction.

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Functional Dissection of an AP-2 β2 Appendage-binding Sequence within the Autosomal Recessive Hypercholesterolemia Protein

Cited by 58 publications

References 58 publications

BRAG2/GEP100/IQSec1 Interacts with Clathrin and Regulates α5β1 Integrin Endocytosis through Activation of ADP Ribosylation Factor 5 (Arf5)

BRAG2/GEP100/IQSec1 Interacts with Clathrin and Regulates α5β1 Integrin Endocytosis through Activation of ADP Ribosylation Factor 5 (Arf5)

Atomic structure of the autosomal recessive hypercholesterolemia phosphotyrosine-binding domain in complex with the LDL-receptor tail

Correcting Estimators of θ and Tajima's D for Ascertainment Biases Caused by the Single-Nucleotide Polymorphism Discovery Process

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