Poly(ornithine)-based self-assembling drug for recovery of hyperammonemia and damage in acute liver injury

Poly(ornithine)-based self-assembling drug for recovery of hyperammonemia and damage in acute liver injury

Oligo-peptides, including monomeric amino acids, have received much attention as bioactive molecules and drugs. One of the biggest problems of these compounds, however, is their very short bioavailability due to instant metabolism and rapid excretion. To solve this problem, we newly designed a poly(...

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Veröffentlicht in:Journal of controlled release 2019-09, Vol.310, p.74-81
Hauptverfasser: Vong, Long B., Ibayashi, Yota, Lee, Yaroslav, Ngo, Dai-Nghiep, Nishikawa, Yuji, Nagasaki, Yukio
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Sprache:eng
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Amino acid
Hyperammonemia
Liver injury
Ornithine
Self-assembling drug
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container_end_page 81
container_issue
container_start_page 74
container_title Journal of controlled release
container_volume 310
creator Vong, Long B.
Ibayashi, Yota
Lee, Yaroslav
Ngo, Dai-Nghiep
Nishikawa, Yuji
Nagasaki, Yukio
description Oligo-peptides, including monomeric amino acids, have received much attention as bioactive molecules and drugs. One of the biggest problems of these compounds, however, is their very short bioavailability due to instant metabolism and rapid excretion. To solve this problem, we newly designed a poly(ethylene glycol) (PEG)-block-polypeptide self-assembling based drug for the treatment of acute liver injury. Here, PEG-block-poly(L-Ornithine) (PEG-b-POrn) was synthesized via a ring opening polymerization, and a nano-sized polyion self-assembling complex (NanoOrn) was prepared by simply mixing polycationic PEG-b-POrn with polyanionic chondroitin sulfate. The obtained NanoOrn was quite stable under high ionic strength and different pH conditions and NanoOrn exhibited extremely low toxicity in vitro and in vivo as compared to the original PEG-b-POrn. As compared to monomeric L-ornithine, administration of NanoOrn to mice significantly improved bioavailability of liberated ornithine, especially in the liver. Interestingly, NanoOrn treatment in acetaminophen (APAP)-induced acute liver injury mice remarkably suppressed blood ammonia levels and liver injury markers, resulting in more effective improvement of liver damage compared to monomeric ornithine via activation of ornithine transcarbomylase. These results show that the self-assembling polypeptide NanoOrn may provide a new concept and promising therapeutics as nanomedicines. [Display omitted]
doi_str_mv 10.1016/j.jconrel.2019.08.011
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One of the biggest problems of these compounds, however, is their very short bioavailability due to instant metabolism and rapid excretion. To solve this problem, we newly designed a poly(ethylene glycol) (PEG)-block-polypeptide self-assembling based drug for the treatment of acute liver injury. Here, PEG-block-poly(L-Ornithine) (PEG-b-POrn) was synthesized via a ring opening polymerization, and a nano-sized polyion self-assembling complex (NanoOrn) was prepared by simply mixing polycationic PEG-b-POrn with polyanionic chondroitin sulfate. The obtained NanoOrn was quite stable under high ionic strength and different pH conditions and NanoOrn exhibited extremely low toxicity in vitro and in vivo as compared to the original PEG-b-POrn. As compared to monomeric L-ornithine, administration of NanoOrn to mice significantly improved bioavailability of liberated ornithine, especially in the liver. 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subjects Amino acid
Hyperammonemia
Liver injury
Ornithine
Self-assembling drug
title Poly(ornithine)-based self-assembling drug for recovery of hyperammonemia and damage in acute liver injury
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