Literature DB >> 18307285

Modulation of antibody pharmacokinetics by chemical polysialylation.

Antony Constantinou1, Agamemnon A Epenetos, Dale Hreczuk-Hirst, Sanjay Jain, Mahendra P Deonarain.   

Abstract

Chemical coupling of a variety of polymers to therapeutic proteins has been studied as a way of improving their pharmacokinetics and pharmacodynamics in vivo. Conjugates have been shown to possess greater stability, lower immunogenicity, and a longer blood circulation time due to the chemicophysical properties of these hydrophilic long chain molecules. Naturally occurring colominic acid (polysialic acid, PSA) has been investigated as an alternative to synthetic polymers such as poly(ethylene glycol) (PEG) due to its lower toxicity and natural metabolism. Antibodies and their fragments are a good example of the types of proteins which benefit from pharmacokinetic engineering. Here, we chemically attached differing amounts and differing lengths of short (11 kDa) and longer (22 kDa) chain colominic acid molecules to the antitumor monoclonal antibody H17E2 Fab fragment. Different coupling ratios and lengths were seen to alter the electrophoretic mobility of the Fab fragment but have a minor effect on the antibody immunoreactivity toward the placental alkaline phosphatase (PLAP) antigen. Polysialylation generally increased Fab fragment blood half-life resulting in higher tumor uptake in a KB human tumor xenograft mouse model. One H17E2 Fab-PSA conjugate had over a 5-fold increase in blood exposure and over a 3-fold higher tumor uptake with only a marginal decrease in tumor/blood selectivity ratio compared to the unconjugated Fab. This conjugate also had a blood bioavailability approaching that of a whole immunoglobulin.

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Year:  2008        PMID: 18307285     DOI: 10.1021/bc700319r

Source DB:  PubMed          Journal:  Bioconjug Chem        ISSN: 1043-1802            Impact factor:   4.774


  9 in total

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Journal:  J Diabetes Sci Technol       Date:  2010-05-01

2.  Engineering the product profile of a polysialyltransferase.

Authors:  Timothy G Keys; Hazel L S Fuchs; Jörg Ehrit; Jürgen Alves; Friedrich Freiberger; Rita Gerardy-Schahn
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Authors:  Núria Sancho Oltra; Praful Nair; Dennis E Discher
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Review 4.  Antibodies targeting cancer stem cells: a new paradigm in immunotherapy?

Authors:  Mahendra P Deonarain; Christina A Kousparou; Agamemnon A Epenetos
Journal:  MAbs       Date:  2009 Jan-Feb       Impact factor: 5.857

Review 5.  Delivery of therapeutic proteins.

Authors:  Dipak S Pisal; Matthew P Kosloski; Sathy V Balu-Iyer
Journal:  J Pharm Sci       Date:  2010-06       Impact factor: 3.534

6.  Understanding the colon cancer stem cells and perspectives on treatment.

Authors:  Elsa N Garza-Treviño; Herminia G Martínez-Rodríguez; Salvador L Said-Fernández
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7.  Different tissue distribution properties for glycosylation variants of fusion proteins containing the p40 subunit of murine interleukin-12.

Authors:  F Bootz; D Venetz; B Ziffels; D Neri
Journal:  Protein Eng Des Sel       Date:  2016-08-11       Impact factor: 1.650

8.  Affinity improvement of a therapeutic antibody by structure-based computational design: generation of electrostatic interactions in the transition state stabilizes the antibody-antigen complex.

Authors:  Masato Kiyoshi; Jose M M Caaveiro; Eri Miura; Satoru Nagatoishi; Makoto Nakakido; Shinji Soga; Hiroki Shirai; Shigeki Kawabata; Kouhei Tsumoto
Journal:  PLoS One       Date:  2014-01-27       Impact factor: 3.240

9.  Anti-inflammatory activity of low molecular weight polysialic acid on human macrophages.

Authors:  Anahita Shahraz; Jens Kopatz; Rene Mathy; Joachim Kappler; Dominic Winter; Shoba Kapoor; Vlad Schütza; Thomas Scheper; Volkmar Gieselmann; Harald Neumann
Journal:  Sci Rep       Date:  2015-11-19       Impact factor: 4.379

  9 in total

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