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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.
Masuda, Yusuke; Yamaguchi, Shinji; Suzuki, Chikako; Aburatani, Takahide; Nagano, Yuki; Miyauchi, Ryuki; Suzuki, Eiko; Yamamura, Naotoshi; Nagatomo, Kentaro; Ishihara, Hidetoshi; Okuno, Kazuaki; Nara, Futoshi; Matschiner, Gabriele; Hashimoto, Ryuji; Takahashi, Tohru; Nishizawa, Tomohiro.
Afiliación
  • Masuda Y; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Yamaguchi S; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Suzuki C; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Aburatani T; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Nagano Y; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Miyauchi R; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Suzuki E; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Yamamura N; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Nagatomo K; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Ishihara H; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Okuno K; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Nara F; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Matschiner G; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Hashimoto R; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Takahashi T; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
  • Nishizawa T; End-Organ Disease Laboratories (Y.M., Y.N., T.N.), Venture Science Laboratories (S.Y.), Modality Research Laboratories (C.S., T.A., R.M., R.H., T.T.), Drug Metabolism & Pharmacokinetics Research Laboratories (E.S., N.Y.), Biologics Technology Research Laboratories (K.N., H.I., K.O.), and Biologi
J Pharmacol Exp Ther ; 365(2): 368-378, 2018 05.
Article en En | MEDLINE | ID: mdl-29463608
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. DS-9001a strongly interfered with PCSK9 binding to low-density-lipoprotein receptor (LDL-R) and PCSK9-mediated degradation of LDL-R. In cynomolgus monkeys, single DS-9001a administration significantly reduced the serum LDL-C level up to 21 days (62.4% reduction at the maximum). Moreover, DS-9001a reduced plasma non-high-density-lipoprotein cholesterol and oxidized LDL levels, and their further reductions were observed when atorvastatin and DS-9001a were administered in combination in human cholesteryl ester transfer protein/ApoB double transgenic mice. Additionally, their reductions on the combination of atorvastatin and DS-9001a were more pronounced than those on the combination of atorvastatin and anacetrapib. Besides its favorable pharmacologic profile, DS-9001a has a lower molecular weight (about 22 kDa), yielding a high stoichiometric drug concentration that might result in a smaller administration volume than that in existing antibody therapy. Since bacterial production systems are viewed as more suited to mass production at low cost, DS-9001a may provide a new therapeutic option to treat patients with dyslipidemia. In addition, considering the growing demand for antibody-like drugs, ABD-fused Anticalin proteins could represent a promising new class of small biologic molecules.
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Texto completo: 1 Banco de datos: MEDLINE Asunto principal: Proteínas Recombinantes de Fusión / Albúminas / Lipocalinas / Proproteína Convertasa 9 Límite: Animals / Humans / Male Idioma: En Revista: J Pharmacol Exp Ther Año: 2018 Tipo del documento: Article
Texto completo
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Texto completo: 1 Banco de datos: MEDLINE Asunto principal: Proteínas Recombinantes de Fusión / Albúminas / Lipocalinas / Proproteína Convertasa 9 Límite: Animals / Humans / Male Idioma: En Revista: J Pharmacol Exp Ther Año: 2018 Tipo del documento: Article