Factor XI Antisense Oligonucleotide for Prevention of Venous Thrombosis

Abstract: BACKGROUND Experimental data indicate that reducing factor XI levels attenuates thrombosis without causing bleeding, but the role of factor XI in the prevention of postoperative venous thrombosis in humans is unknown. FXI-ASO (ISIS 416858) is a second-generation antisense oligonucleotide that specifically reduces factor XI levels. We compared the efficacy and safety of FXI-ASO with those of enoxaparin in patients undergoing total knee arthroplasty. METHODS In this open-label, parallel-group study, we randoml… Show more

“…However, in patients at or above the 80th percentile, corresponding to ‫ف‬ 50 mg/dl plasma Lp(a) concentrations, much greater reduction than is currently achieved with these indirect therapeutic agents would be required to signifi cantly reduce CVD risk, which is thought to occur at levels which exceed [25][26][27][28][29][30] or OxPL-apoB concentrations, consistent with the independence of lowering of Lp(a) and OxPL-apoB on isoform size ( Fig. 8 ).…”

“…1 ). These drugs also have an improved therapeutic index due to reduced pro-infl ammatory properties (22)(23)(24)(25)(26).…”

Antisense inhibition of apolipoprotein (a) to lower plasma lipoprotein (a) levels in humans

“…However, in patients at or above the 80th percentile, corresponding to ‫ف‬ 50 mg/dl plasma Lp(a) concentrations, much greater reduction than is currently achieved with these indirect therapeutic agents would be required to signifi cantly reduce CVD risk, which is thought to occur at levels which exceed [25][26][27][28][29][30] or OxPL-apoB concentrations, consistent with the independence of lowering of Lp(a) and OxPL-apoB on isoform size ( Fig. 8 ).…”

“…1 ). These drugs also have an improved therapeutic index due to reduced pro-infl ammatory properties (22)(23)(24)(25)(26).…”

Antisense inhibition of apolipoprotein (a) to lower plasma lipoprotein (a) levels in humans

“…[24][25][26] Recently, a phase 2 trial demonstrated that FXI-antisense oligonucleotide (FXI-ASO) reduced FXI levels and decreased the incidence of deep vein thrombosis (DVT) after knee arthroplasty without increasing bleeding, thus providing evidence that FXIa can contribute to thrombosis in humans. 27 However, postoperative bleeding in knee arthroplasty is relatively uncommon, and the rate of bleeding with FXI-ASO was not significantly lower than that seen with enoxaparin. 28,29 The FXI-ASO trial demonstrated a role for FXIa in DVT but did not resolve the role of either platelet polyP or FXIIa in postarthroplasty DVT because FXIa can inactivate tissue factor pathway inhibitor, 30 and FXI can be feedback-activated by thrombin.…”

FXIa and platelet polyphosphate as therapeutic targets during human blood clotting on collagen/tissue factor surfaces under flow

“…RNase Hactive ASOs targeting the disease-associated proteins ApoB100, APOCIII, and FXI have produced dosedependent pharmacology in humans, and, in several cases, near complete depletion of these liverderived proteins from plasma has been achieved. [66][67][68][69] Importantly, Kynamro TM , the generation-2 ASO targeting ApoB100, was recently approved for the treatment of homozygous familial hypercholesterolemia, making it the first FDA-approved systemically delivered antisense drug. 67 Moreover, robust clinical efficacy of additional generation-2 ASOs including those targeting APOCIII in the triglyceride pathway and FXI, a regulator of thrombosis, has recently been reported in 2 separate seminal articles in The New England Journal of Medicine.…”

“…67 Moreover, robust clinical efficacy of additional generation-2 ASOs including those targeting APOCIII in the triglyceride pathway and FXI, a regulator of thrombosis, has recently been reported in 2 separate seminal articles in The New England Journal of Medicine. 68,69 As mentioned above, recent advances continue to further the pharmacologic properties, potency, and selectivity of ASO technology and have led to the discovery and clinical evaluation of next-generation cEt ASOs and GalNAc-conjugated ASOs that hold tremendous potential to modulate difficult-to-drug targets in many disease indications including cancer.…”

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