2018
DOI: 10.1124/jpet.117.246652
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Generation and Characterization of a Novel Small Biologic Alternative to Proprotein Convertase Subtilisin/Kexin Type 9 (PCSK9) Antibodies, DS-9001a, Albumin Binding Domain–Fused Anticalin Protein

Abstract: Since it was recently reported that an antibody for proprotein convertase subtilisin/kexin type 9 (PCSK9) reduces the risk of cardiovascular events in a clinical context, PCSK9 inhibition is thought to be an attractive therapy for dyslipidemia. In the present study, we created a novel small biologic alternative to PCSK9 antibodies called DS-9001a, comprising an albumin binding domain fused to an artificial lipocalin mutein (ABD-fused Anticalin protein), which can be produced by a microbial production system. D… Show more

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Cited by 38 publications
(21 citation statements)
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“…Unfortunately in humans this construct reduced LDL-C by only 47% at the highest intravenous dose, or by 48% as a subcutaneous dose in combination with statins [82], in stark contrast to the efficacy of approved antibodies such as Evolocumab which reduce cholesterol by 60% or more with similar doses [79]. Alongside this work, an affibody non-antibody domain which targeted PCSK9 was fused with serum albumin for longer half-life [79,83]. In a similar application, and to further improve efficacy, a serum albumin domain was also fused to the Adnectin-anti-PCSK9 construct to improve circulation half-life to match that of antibodies ( Figure 3E) [79].…”
Section: Fusion To Extend Half-lifementioning
confidence: 99%
“…Unfortunately in humans this construct reduced LDL-C by only 47% at the highest intravenous dose, or by 48% as a subcutaneous dose in combination with statins [82], in stark contrast to the efficacy of approved antibodies such as Evolocumab which reduce cholesterol by 60% or more with similar doses [79]. Alongside this work, an affibody non-antibody domain which targeted PCSK9 was fused with serum albumin for longer half-life [79,83]. In a similar application, and to further improve efficacy, a serum albumin domain was also fused to the Adnectin-anti-PCSK9 construct to improve circulation half-life to match that of antibodies ( Figure 3E) [79].…”
Section: Fusion To Extend Half-lifementioning
confidence: 99%
“…A recent alternative biologic approach was to use a 22 kDa albuminbinding domain (ABD)-fused Anticalin protein DS-9001a produced in bacteria (Figure 2). 34 In cynomolgus monkeys, a single subcutaneous injection of such ABD-fused Anticalin protein was reported to have a somewhat longer half-life in plasma (120h) 34 compared to mAbs (60-120 h) 91 and BMS-962476 (74-108 h). 33 Such treatment resulted in a sustained 50-60% reduction of LDL-C lasting up to 21 days (Table 1), and its effect was significantly potentiated by atorvastatin.…”
Section: Other Inhibitors Of Pcsk9-ldlr Bindingmentioning
confidence: 99%
“…Adenoviral overexpression of AnxA2 in the liver results in an increase of LDLR expression [26]; (2) DS-9001a is a small biologic molecule, composed of an albumin-binding domain fused with an artificial lipocalin mutein enabling high specific recognition of the target protein. DS-9001a inhibits the binding of the PCSK9 to LDLR, preventing LDLR degradation [27]; (3) Adnectin, BMS-962,476 is a PCSK9-targeting polypeptide conjugated with polyethylene glycol which enhances its pharmacokinetic profile, binding to human PCSK9 with subnanomolar affinity. Adnectin hinders the interaction between the EGF-A domain of LDLR and extracellular PCSK9, thus preventing the PCSK9-induced degradation of LDLR [28].…”
Section: Article Highlightsmentioning
confidence: 99%