Andreas Bernkop‐Schnürch scite author profile

Due to the obvious advantages of long-acting peptide and protein drugs, strategies to prolong plasma half life time of such compounds are highly on demand. Short plasma half life times are commonly due to fast renal clearance as well as to enzymatic degradation occurring during systemic circulation. Modifications of the peptide/protein can lead to prolonged plasma half life times. By shortening the overall amino acid amount of somatostatin and replacing L: -analogue amino acids with D: -amino acids, plasma half life time of the derivate octreotide was 1.5 hours in comparison to only few minutes of somatostatin. A PEG(2,40 K) conjugate of INF-alpha-2b exhibited a 330-fold prolonged plasma half life time compared to the native protein. It was the aim of this review to provide an overview of possible strategies to prolong plasma half life time such as modification of N- and C-terminus or PEGylation as well as methods to evaluate the effectiveness of drug modifications. Furthermore, fundamental data about most important proteolytic enzymes of human blood, liver and kidney as well as their cleavage specificity and inhibitors for them are provided in order to predict enzymatic cleavage of peptide and protein drugs during systemic circulation.

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Chitosan-based drug delivery systems

Bernkop‐Schnürch

Dünnhaupt

2012

European Journal of Pharmaceutics and Biopharmaceutics

805

412

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Thiomers: A new generation of mucoadhesive polymers

Bernkop‐Schnürch

2005

Advanced Drug Delivery Reviews

550

273

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Comparison of the mucoadhesive properties of various polymers

Grabovac

Guggi

Bernkop‐Schnürch

2005

Advanced Drug Delivery Reviews

384

201

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Thiolated polymers — thiomers: development and in vitro evaluation of chitosan–thioglycolic acid conjugates

2001

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