Ligand Design with Accelerated Disulfide Formation with Serum Albumin to Extend Blood Retention

Song Qi; Zixuan Liu; Keitaro Suyama; Yuichi Tsuchiya; Jedidiah Canarejo; Khanh Quoc Phan; Noriko Yutsudo; Atsushi Shimada; Takeshi Hirota; Ichiro Ieiri; Akihiro Kishimura; Takahiro Muraoka; Takeru Nose; Takeshi Mori; Yoshiki Katayama

doi:10.1021/acsmedchemlett.4c00503

Ligand Design with Accelerated Disulfide Formation with Serum Albumin to Extend Blood Retention

Song Qi, Zixuan Liu, Keitaro Suyama, Yuichi Tsuchiya, Jedidiah Canarejo, Khanh Quoc Phan, Noriko Yutsudo, Atsushi Shimada, Takeshi Hirota, Ichiro Ieiri, Akihiro Kishimura, Takahiro Muraoka, Takeru Nose, Takeshi Mori, Yoshiki Katayama

研究成果: ジャーナルへの寄稿 › 学術誌 › 査読

抄録

We proposed a novel ligand for the interaction with human serum albumin (HSA) to extend the blood half-life of small molecular weight therapeutics. The ligand features an alkyl chain and an activated disulfide to allow binding to the hydrophobic pockets of HSA and the formation of disulfide to Cys34 of HSA, thereby minimizing the initial renal clearance. The dual nature of the ligand-HSA bonding was expected to give the ligand long blood retention. After 1 min of mixing with HSA, the ligand showed higher binding (1.7 times) than that of a control ligand (containing only activated disulfide). After intravenous injection to mice, the ligand half-lives were 1.6 and 9.2 times longer than those of control ligands with the active disulfide alone and with the alkyl chain alone, respectively. The proposed ligand has the potential to act as a platform for extending the half-life of small therapeutics in vivo.

本文言語	英語
ページ（範囲）	144-148
ページ数	5
ジャーナル	ACS Medicinal Chemistry Letters
巻	16
号	1
DOI	https://doi.org/10.1021/acsmedchemlett.4c00503
出版ステータス	出版済み - 1月 9 2025

!!!All Science Journal Classification (ASJC) codes

生化学
創薬
有機化学

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Qi, S., Liu, Z., Suyama, K., Tsuchiya, Y., Canarejo, J., Phan, K. Q., Yutsudo, N., Shimada, A., Hirota, T., Ieiri, I., Kishimura, A., Muraoka, T., Nose, T., Mori, T., & Katayama, Y. (2025). Ligand Design with Accelerated Disulfide Formation with Serum Albumin to Extend Blood Retention. ACS Medicinal Chemistry Letters, 16(1), 144-148. https://doi.org/10.1021/acsmedchemlett.4c00503

Qi, S, Liu, Z, Suyama, K, Tsuchiya, Y, Canarejo, J, Phan, KQ, Yutsudo, N , Shimada, A , Hirota, T, Ieiri, I, Kishimura, A, Muraoka, T, Nose, T , Mori, T & Katayama, Y 2025, 'Ligand Design with Accelerated Disulfide Formation with Serum Albumin to Extend Blood Retention', ACS Medicinal Chemistry Letters, vol. 16, no. 1, pp. 144-148. https://doi.org/10.1021/acsmedchemlett.4c00503

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abstract = "We proposed a novel ligand for the interaction with human serum albumin (HSA) to extend the blood half-life of small molecular weight therapeutics. The ligand features an alkyl chain and an activated disulfide to allow binding to the hydrophobic pockets of HSA and the formation of disulfide to Cys34 of HSA, thereby minimizing the initial renal clearance. The dual nature of the ligand-HSA bonding was expected to give the ligand long blood retention. After 1 min of mixing with HSA, the ligand showed higher binding (1.7 times) than that of a control ligand (containing only activated disulfide). After intravenous injection to mice, the ligand half-lives were 1.6 and 9.2 times longer than those of control ligands with the active disulfide alone and with the alkyl chain alone, respectively. The proposed ligand has the potential to act as a platform for extending the half-life of small therapeutics in vivo.",

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doi = "10.1021/acsmedchemlett.4c00503",

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AU - Canarejo, Jedidiah

AU - Phan, Khanh Quoc

AU - Yutsudo, Noriko

AU - Shimada, Atsushi

AU - Hirota, Takeshi

AU - Ieiri, Ichiro

AU - Kishimura, Akihiro

AU - Muraoka, Takahiro

AU - Nose, Takeru

AU - Mori, Takeshi

AU - Katayama, Yoshiki

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N2 - We proposed a novel ligand for the interaction with human serum albumin (HSA) to extend the blood half-life of small molecular weight therapeutics. The ligand features an alkyl chain and an activated disulfide to allow binding to the hydrophobic pockets of HSA and the formation of disulfide to Cys34 of HSA, thereby minimizing the initial renal clearance. The dual nature of the ligand-HSA bonding was expected to give the ligand long blood retention. After 1 min of mixing with HSA, the ligand showed higher binding (1.7 times) than that of a control ligand (containing only activated disulfide). After intravenous injection to mice, the ligand half-lives were 1.6 and 9.2 times longer than those of control ligands with the active disulfide alone and with the alkyl chain alone, respectively. The proposed ligand has the potential to act as a platform for extending the half-life of small therapeutics in vivo.

AB - We proposed a novel ligand for the interaction with human serum albumin (HSA) to extend the blood half-life of small molecular weight therapeutics. The ligand features an alkyl chain and an activated disulfide to allow binding to the hydrophobic pockets of HSA and the formation of disulfide to Cys34 of HSA, thereby minimizing the initial renal clearance. The dual nature of the ligand-HSA bonding was expected to give the ligand long blood retention. After 1 min of mixing with HSA, the ligand showed higher binding (1.7 times) than that of a control ligand (containing only activated disulfide). After intravenous injection to mice, the ligand half-lives were 1.6 and 9.2 times longer than those of control ligands with the active disulfide alone and with the alkyl chain alone, respectively. The proposed ligand has the potential to act as a platform for extending the half-life of small therapeutics in vivo.

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KW - Extension of blood retention

KW - Human serum albumin

KW - Hydrophobic interaction

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Ligand Design with Accelerated Disulfide Formation with Serum Albumin to Extend Blood Retention

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