Polymers for Protein Conjugation

Pasut, Gianfranco

doi:10.3390/polym6010160

Cited by 69 publications

(50 citation statements)

References 95 publications

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“…The conjugation of polymers to drugs is a well-established strategy in drug delivery to enhance the solubility of the drug and increase the circulation time in the body, while at the same time lowering the immunogenicity [29]. The versatility and potential of PEtOX as an alternative to PEO were also demonstrated for both protein and smalldrug conjugates; comparable results were obtained for PEtOX and PEO in regard to, for example, protein-rejecting properties, drug-release profile, and in vitro cytotoxicity [75][76][77][78].…”

Section: Responsivity To Temperaturementioning

confidence: 97%

Smart polymers in drug delivery systems on crossroads: Which way deserves following?

Hrubý

Filippov

Štěpánek

2015

European Polymer Journal

119

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Section: Responsivity To Temperaturementioning

confidence: 97%

Smart polymers in drug delivery systems on crossroads: Which way deserves following?

Hrubý

Filippov

Štěpánek

2015

European Polymer Journal

119

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“…For example, although PEG is often considered an "inert" polymer, high molar mass PEG is not degraded in vivo and can cause toxicity, as can high doses of PEG polymers of low molar mass. [82][83][84][85] Immunogenic response to PEG has been reported. 84,86 Furthermore, synthetic PEG may contain impurities or unreacted monomer which is highly toxic.…”

Section: Peptide Hydrogelsmentioning

confidence: 99%

Self-assembly of bioactive peptides, peptide conjugates, and peptide mimetic materials

2017

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Molecular self-assembly is a multi-disciplinary field of research, with potential chemical and biological applications. One of the main driving forces of self-assembly is molecular amphiphilicity, which can drive formation of complex and stable nanostructures. Self-assembling peptide and peptide conjugates have attracted great attention due to their biocompatibility, biodegradability and biofunctionality. Understanding assembly enables the better design of peptide amphiphiles which may form useful and functional nanostructures. This review covers self-assembly of amphiphilic peptides and peptide mimetic materials, as well as their potential applications. Peptide self-assemblySelf-assembly is defined as the ability of a molecule, without guidance of external factors, to associate through non-covalent interactions to form highly ordered 3-dimensional structures.

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“…This developing area is considered as one of the most important breakthroughs in biological drug development (Pasut 2014b ), offering multiple advantages over the chemical coupling with synthetic polymers. In particular, two distinct technologies have emerged, PASylation ® ) and XTEN ™ (Schellenberger et al 2009 ), which both employ recombinant polypeptides to mimic the size-enlarging effect of PEG for plasma half-life extension.…”

Section: Genetic Fusion With Recombinant Biopolymersmentioning

confidence: 99%

Biobetters

2015

AAPS Advances in the Pharmaceutical Sciences Series

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Polymers for Protein Conjugation

Cited by 69 publications

References 95 publications

Smart polymers in drug delivery systems on crossroads: Which way deserves following?

Smart polymers in drug delivery systems on crossroads: Which way deserves following?

Self-assembly of bioactive peptides, peptide conjugates, and peptide mimetic materials

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