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Albumin Fusion at the N-Terminus or C-Terminus of HM-3 Leads to Improved Pharmacokinetics and Bioactivities.


ABSTRACT: HM-3, an integrin antagonist, exhibits anti-tumor biological responses and therefore has potential as a therapeutic polypeptide. However, the clinical applications of HM-3 are limited by its short half-life. In this study, we genetically fused human serum albumin (HSA) to the N or C-terminus of HM-3 to improve HM-3 pharmacokinetics. HM-3/HSA proteins were successfully expressed in Pichia pastoris and displayed improved pharmacokinetic properties and stability. Among them, the half-life of HM-3-HSA was longer than HSA-HM-3. In vitro, the IC50 values of HSA-HM-3 and HM-3-HSA were 0.38 ± 0.14 μM and 0.25 ± 0.08 μM in B16F10 cells, respectively. In vivo, the inhibition rates of B16F10 tumor growth were 36% (HSA-HM-3) and 56% (HM-3-HSA), respectively, indicating antitumor activity of HM-3-HSA was higher than HSA-HM-3. In conclusion, these results suggested that the HM-3/HSA fusion protein might be potential candidate HM-3 agent for treatment of melanoma and when HSA was fused at the C-terminus of HM-3, the fusion protein had a higher stability and activity.

SUBMITTER: Li T 

PROVIDER: S-EPMC8472738 | biostudies-literature | 2021 Aug

REPOSITORIES: biostudies-literature

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Albumin Fusion at the N-Terminus or C-Terminus of HM-3 Leads to Improved Pharmacokinetics and Bioactivities.

Li Ting T   Zhang Han-Zi HZ   Ge Guang-Fei GF   Yue Zhao-Rong ZR   Wang Ru-Yue RY   Zhang Qian Q   Gu Yan Y   Song Mei-Juan MJ   Li Wen-Bo WB   Ma Min-Zhi MZ   Wang Mei-Zhu MZ   Yang Hui H   Li Yang Y   Li Hong-Yu HY  

Biomedicines 20210825 9


HM-3, an integrin antagonist, exhibits anti-tumor biological responses and therefore has potential as a therapeutic polypeptide. However, the clinical applications of HM-3 are limited by its short half-life. In this study, we genetically fused human serum albumin (HSA) to the N or C-terminus of HM-3 to improve HM-3 pharmacokinetics. HM-3/HSA proteins were successfully expressed in <i>Pichia pastoris</i> and displayed improved pharmacokinetic properties and stability. Among them, the half-life of  ...[more]

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