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Structure-based engineering of an antiangiogenic scFv antibody for soluble production in E. coli without loss of activity

  • Melis Denizci Öncü*
  • , Bertan Koray Balcıoğlu
  • , Beytullah Özgür
  • , Hasan Ümit Öztürk
  • , Müge Serhatlı
  • , Şeyma Işık
  • , Berrin Erdağ
  • , Gizem Dinler Doğanay
  • , Aylin Özdemir Bahadır
  • *Bu çalışma için yazışmadan sorumlu yazar

Araştırma sonucu: Dergiye katkıMakalebilirkişi

6 Atıf (Scopus)

Özet

Development of monoclonal antibody therapeutics against vascular endothelial growth factor receptor 2 (VEGFR-2) protein, which is the main regulator in angiogenesis, has been a major challenge for years. In the current study, we engineer an inclusion body forming single-chain variable fragment (scFv) against VEGFR-2 by using complementarity determining regions (CDR) grafting technique to improve its solubility and investigate the activity of the engineered molecule. CDR sequences of the target scFv were grafted into the framework of another intrinsically soluble scFv molecule. Based on the computational results, CDR grafting has increased the solubility of the grafted scFv molecule. Results confirmed that the grafting approach increased in vivo folding properties of the target scFv molecule compared with the original scFv molecule. Similar binding affinities to the VEGFR-2 were observed for the original and the grafted scFv by surface plasmon resonance assays. Biological activity assays, including human umbilical vein endothelial cells proliferation and wound healing assays, showed that grafted scFv molecule has an antiangiogenic property. This study suggests that an antiangiogenic scFv fully expressed as an inclusion body can be rescued by grafting its CDR regions to a scFv expressed in a soluble form without any loss in its binding property and its activity.

Orijinal dilİngilizce
Sayfa (başlangıç-bitiş)2122-2137
Sayfa sayısı16
DergiBiotechnology and Applied Biochemistry
Hacim69
Basın numarası5
DOI'lar
Yayın durumuYayınlandı - Eki 2022

Bibliyografik not

Publisher Copyright:
© 2021 International Union of Biochemistry and Molecular Biology, Inc.

Finansman

This work was partially supported by different grants from TUBITAK 1009 TARAL project (117H001) and TUBITAK TARAL 1003 project (216S387). H L informationThis work was partially supported by different grants from TUBITAK 1009 TARAL project (117H001) and TUBITAK TARAL 1003 project (216S387).

FinansörlerFinansör numarası
TUBITAK
TUBITAK TARAL 1003 project216S387
Türkiye Bilimsel ve Teknolojik Araştırma Kurumu117H001

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