Abstract
PCSK9 is a protein secreted by the liver that binds to the low-density lipoprotein receptor (LDLR), causing LDLR internalization, decreasing the clearance of circulating LDL particles. Mutations in PCSK9 that strengthen its interactions with LDLR result in familial hypercholesterolemia (FH) and early onset atherosclerosis, while nonsense mutations of PCSK9 result in cardio-protective hypocholesterolemia. These observations led to PCSK9 inhibition for cholesterol lowering becoming a high-interest therapeutic target, with antibody drugs reaching the market. An orally-available small molecule drug is highly desirable, but inhibiting the PCSK9/LDLR protein-protein interaction (PPI) has proven challenging. Alternate approaches to finding good lead candidates are needed. Motivated by the FH mutation data on PCSK9, we found that modeling the PCSK9/LDLR interface revealed extensive electron delocalization between and within the protein partners. Based on this, we hypothesized that compounds assembled from chemical fragments could achieve the affinity required to inhibit the PCSK9/LDLR PPI if they were selected to interact with PCSK9 in a way that, like LDLR, also involves significant fractional charge transfer to form partially covalent bonds. To identify such fragments, Simulated Annealing of Chemical Potential (SACP) fragment simulations were run on multiple PCSK9 structures, using optimized partial charges for the protein. We designed a small molecule, composed of several fragments, predicted to interact at two sites on the PCSK9. This compound inhibits the PPI with 1 μM affinity. Further, we designed two similar small molecules where one allows charge delocalization though a linker and the other doesn’t. The first inhibitor with charge delocalization enhances LDLR surface expression by 60% at 10 nM, two orders of magnitude more potent than the EGF domain of LDLR. The other enhances LDLR expression by only 50% at 1 μM. This supports our conjecture that fragments can have surprisingly outsized efficacy in breaking PPI’s by achieving fractional charge transfer leading to partially covalent bonding.
Highlights
Efficient removal of LDL particles from the blood stream is an essential process for preventing hypercholesterolemia and its associated atherosclerosis
GAMESS/RESP calculations indicate that it is possible to attain high affinity binding at the T377-R194-D238 locus with a small molecule by tapping into the intrinsic electron delocalization propensity from this site through the D374-R218 locus of PCSK9 that is seen upon binding to low-density lipoprotein receptor (LDLR)
The large area of PCSK9 that can be called the LDLR Ca2+ ion site, does not bind any fragments with high affinity according to Simulated Annealing of Chemical Potential (SACP), and is strongly hydrated according to solvation calculations
Summary
Efficient removal of LDL particles from the blood stream is an essential process for preventing hypercholesterolemia and its associated atherosclerosis. The key to translating basic research into practical drug discovery is target validation This was achieved for PCSK9[21,22,23,24,25,26,27] with the finding that inactivating mutations resulted in individuals with low blood cholesterol, a history of no coronary artery disease, and, most importantly, no deleterious side effects. It would obviously be highly desirable to have orally-available small molecule inhibitors of the PSCK9/LDLR interaction, because such compounds have the potential to be much more cost effective to produce than protein antibodies Analysis of this structure indicates that there are 4 key interaction (Fig 2) sites that span a large distance
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