Structural and Biochemical Characterization of the Wild Type PCSK9-EGF(AB) Complex and Natural Familial Hypercholesterolemia Mutants

Bottomley, M.J.; Cirillo, Agostino; Orsatti, Laura; Ruggeri, Lionello; Fisher, Timothy S.; Santoro, Joseph C.; Cummings, Richard; Cubbon, Rose M.; Surdo, Paola Lo; Calzetta, Alessandra; Noto, Alessia; Baysarowich, Jennifer; Mattu, Marco; Talamo, Fabio; Francesco, Raffaele De; Sparrow, Carl P.; Sitlani, Ayesha; Carfı́, Andrea

doi:10.1074/jbc.m808363200

Cited by 117 publications

(137 citation statements)

References 38 publications

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“…4), in agreement with its reported enhanced LDLR-binding affinity at neutral pH (11,18,23). Concentrations of secreted PCSK9, up to 12 nM (HepG2 cells; ϳ3ϫ endogenous levels; Fig.…”

Section: Discussionsupporting

confidence: 74%

“…Inhibition of the PCSK9-induced LDLR Degradation by EGF-AB-An EGF-AB peptide containing the LDLR binding site to PCSK9 was reported to inhibit the effect of exogenously added PCSK9 on LDLR degradation in either HEK293 or HepG2 cells (18,23,24). Although the effect of WT EGF-AB on naïve HepG2 cells was not reported, the inhibitory effect of the gain-of-function EGF-AB H306Y is best seen with exogenous PCSK9, with little effect on naïve HepG2 cells (18).…”

Section: Blockade Of Endocytosis In Hepg2 Cells Does Not Affectmentioning

confidence: 99%

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Dissection of the Endogenous Cellular Pathways of PCSK9-induced Low Density Lipoprotein Receptor Degradation

Poirier

Mayer

Poupon

et al. 2009

Journal of Biological Chemistry

234

185

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Elevated levels of plasma low density lipoprotein (LDL)-cholesterol, leading to familial hypercholesterolemia, are enhanced by mutations in at least three major genes, the LDL receptor (LDLR), its ligand apolipoprotein B, and the proprotein convertase PCSK9. Single point mutations in PCSK9 are associated with either hyperor hypocholesterolemia. Accordingly, PCSK9 is an attractive target for treatment of dyslipidemia. PCSK9 binds the epidermal growth factor domain A (EGF-A) of the LDLR and directs it to endosomes/ lysosomes for destruction. Although the mechanism by which PCSK9 regulates LDLR degradation is not fully resolved, it seems to involve both intracellular and extracellular pathways. Here, we show that clathrin light chain small interfering RNAs that block intracellular trafficking from the trans-Golgi network to lysosomes rapidly increased LDLR levels within HepG2 cells in a PCSK9-dependent fashion without affecting the ability of exogenous PCSK9 to enhance LDLR degradation. In contrast, blocking the extracellular LDLR endocytosis/degradation pathway by a 4-, 6-, or 24-h incubation of cells with Dynasore or an EGF-AB peptide or by knockdown of endogenous autosomal recessive hypercholesterolemia did not significantly affect LDLR levels. The present data from HepG2 cells and mouse primary hepatocytes favor a model whereby depending on the dose and/or incubation period, endogenous PCSK9 enhances the degradation of the LDLR both extraand intracellularly. Therefore, targeting either pathway, or both, would be an effective method to reduce PCSK9 activity in the treatment of hypercholesterolemia and coronary heart disease.

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“…4), in agreement with its reported enhanced LDLR-binding affinity at neutral pH (11,18,23). Concentrations of secreted PCSK9, up to 12 nM (HepG2 cells; ϳ3ϫ endogenous levels; Fig.…”

Section: Discussionsupporting

confidence: 74%

Section: Blockade Of Endocytosis In Hepg2 Cells Does Not Affectmentioning

confidence: 99%

Dissection of the Endogenous Cellular Pathways of PCSK9-induced Low Density Lipoprotein Receptor Degradation

Poirier

Mayer

Poupon

et al. 2009

Journal of Biological Chemistry

234

185

View full text Add to dashboard Cite

show abstract

“…Various approaches include humanized monoclonal antibodies, antisense oligonucleotides, RNA interference, and small molecule inhibitors. Recent success in studies with antibodies directed against PCSK9 has further increased interest in this target (19,20). As progress toward therapeutic intervention of PCSK9-LDLR interactions advances, it is important to understand the molecular basis of the biological events involved.…”

Section: Discussionmentioning

confidence: 99%

A Two-step Binding Model of PCSK9 Interaction with the Low Density Lipoprotein Receptor

Yamamoto¹,

Lu²,

Ryan³

2011

Journal of Biological Chemistry

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PCSK9 (proprotein convertase subtilisin-like/kexin type 9) is an emerging target for pharmaceutical intervention. This multidomain protein interacts with the LDL receptor (LDLR), promoting receptor degradation. Insofar as PCSK9 inhibition induces a decrease in plasma cholesterol levels, understanding the nature of the binding interaction between PCSK9 and the LDLR is of critical importance. In this study, the ability of PCSK9 to compete with apoE3 N-terminal domain-containing reconstituted HDL for receptor binding was examined. Whereas full-length PCSK9 was an effective competitor, the N-terminal domain (composed of the prodomain and catalytic domain) was not. Surprisingly, the C-terminal domain (CT domain) of PCSK9 was able to compete. Using a direct binding interaction assay, we show that the PCSK9 CT domain bound to the LDLR in a calcium-dependent manner and that co-incubation with the prodomain and catalytic domain had no effect on this binding. To further characterize this interaction, two LDLR fragments, the classical ligand-binding domain (LBD) and the EGF precursor homology domain, were expressed in stably transfected HEK 293 cells and isolated. Binding assays showed that the PCSK9 CT domain bound to the LBD at pH 5.4. Thus, CT domain interaction with the LBD of the LDLR at endosomal pH constitutes a second step in the PCSK9-mediated LDLR binding that leads to receptor degradation.

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“…In addition, the structure determination of the complex under different pH conditions has suggested that the His-306 of EGF-A forms an additional salt bridge with the Asp-374 of PCSK9 at acidic pH (McNutt et al 2009), which should stabilize the PCSK9-LDLR complex under acidic conditions. In fact, the mutation of His-306 to Tyr is known to be associated with FH (Day et al 1997), and crystallographic analysis has demonstrated that the hydroxyl group of Tyr forms a stable hydrogen bond with Asp-374 even at neutral pH (Bottomley et al 2009;McNutt et al 2009). …”

Section: Asp-70mentioning

confidence: 99%

“…The structure determination of the EGF-AB pair in complex with PCSK9 has shown that the calcium-binding site of EGF-A serves as the binding site for PCSK9 (Bottomley et al 2009;Kwon et al 2008;McNutt et al 2009) (Fig. 3b).…”

Section: Asp-70mentioning

confidence: 99%

How multi-scale structural biology elucidated context-dependent variability in ectodomain conformation along with the ligand capture and release cycle for LDLR family members

Nogi

2017

Biophys Rev

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The low-density lipoprotein receptor (LDLR) and its homologs capture and internalize lipoproteins into the cell. Due to the fact that LDLR family members possess a modular ectodomain that undergoes dynamic conformational changes, multi-scale structural analysis has been performed so as to understand the ligand capture and release mechanism. For example, crystallographic analyses have provided models for both the entire ectodomain and high-resolution structures of individual modules. In addition, nuclear magnetic resonance spectroscopic analyses have shown the rigidity and flexibility of inter-module linkers to restrict the mobility of ectodomain. Accumulated structural data suggest that the ectodomains of LDLR family members are flexible at the cell surface and switch between two metastable conformations, that is, the extended and contracted conformations. Recent structural analysis of ApoER2, a close homolog of LDLR, raised the possibility that the receptor binds with the ligand in the contracted conformation. After transport to an endosome by endocytosis, the receptor undergoes a conformational change to the closed conformation for completion of ligand release. In contrast, LDLR has been reported to adopt the extended conformation when it binds with a inhibitory regulator that recruits LDLR toward the degradation pathway. These findings support a mechanism of different ectodomain conformations for binding the ligand versus binding the regulatory protein. In this review, I provide an overview of studies that analyze the structural and biophysical properties of the ectodomains of LDLR family members and discuss a hypothetical model for ligand uptake and receptor recycling that integrates the known ectodomain conformational variability.

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Structural and Biochemical Characterization of the Wild Type PCSK9-EGF(AB) Complex and Natural Familial Hypercholesterolemia Mutants

Cited by 117 publications

References 38 publications

Dissection of the Endogenous Cellular Pathways of PCSK9-induced Low Density Lipoprotein Receptor Degradation

Dissection of the Endogenous Cellular Pathways of PCSK9-induced Low Density Lipoprotein Receptor Degradation

A Two-step Binding Model of PCSK9 Interaction with the Low Density Lipoprotein Receptor

How multi-scale structural biology elucidated context-dependent variability in ectodomain conformation along with the ligand capture and release cycle for LDLR family members

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