Transforming waste into valuables: Preparation and evaluation of dual-ligand hydrophobic charge-induction chromatography using two poor performing ligands

Wei Shi; Tian-Yi Zhang; Chao-Ying Fang; Si-Qi Zhang; Kai-Bin Li; Xiao-Bin Zhang; De-Man Han

doi:10.1016/j.chroma.2024.464975

Transforming waste into valuables: Preparation and evaluation of dual-ligand hydrophobic charge-induction chromatography using two poor performing ligands

J Chromatogr A. 2024 Jul 5:1726:464975. doi: 10.1016/j.chroma.2024.464975. Epub 2024 May 8.

Authors

Wei Shi¹, Tian-Yi Zhang², Chao-Ying Fang², Si-Qi Zhang², Kai-Bin Li², Xiao-Bin Zhang², De-Man Han³

Affiliations

¹ School of Pharmaceutical and Chemical Engineering, Taizhou University, Jiaojiang 318000, China; Taizhou Research Institute of Bio-Medical and Chemical Industry CO., LTD, Jiaojiang 318000, China.
² School of Pharmaceutical and Chemical Engineering, Taizhou University, Jiaojiang 318000, China.
³ School of Pharmaceutical and Chemical Engineering, Taizhou University, Jiaojiang 318000, China. Electronic address: hdmtzc@126.com.

PMID: 38735118
DOI: 10.1016/j.chroma.2024.464975

Abstract

In conventional chromatographic ligand screening, underperforming ligands are often dismissed. However, this practice may inadvertently overlook potential opportunities. This study aims to investigate whether these underperforming ligands can be repurposed as valuable assets. Hydrophobic charge-induction chromatography (HCIC) is chosen as the validation target for its potential as an innovative chromatographic mode. A novel dual-ligand approach is employed, combining two suboptimal ligands (5-Aminobenzimidazole and Tryptamine) to explore enhanced performance and optimization prospects. Various dual-ligand HCIC resins with different ligand densities were synthesized by adjusting the ligand ratio and concentration. The resins were characterized to assess appearance, functional groups, and pore features using SEM, FTIR, and ISEC techniques. Performance assessments were conducted using single-ligand mode resins as controls, evaluating the selectivity against human immunoglobulin G and human serum albumin. Static adsorption experiments were performed to understand pH and salt influence on adsorption. Breakthrough experiments were conducted to assess dynamic adsorption capacity of the novel resin. Finally, chromatographic separation using human serum was performed to evaluate the purity and yield of the resin. Results indicated that the dual-ligand HCIC resin designed for human antibodies demonstrates exceptional selectivity, surpassing not only single ligand states but also outperforming certain high-performing ligand types, particularly under specific salt and pH conditions. Ultimately, a high yield of 83.9 % and purity of 96.7 % were achieved in the separation of hIgG from human serum with the dual-ligand HCIC, significantly superior to the single-ligand resins. In conclusion, through rational design and proper operational conditions, the dual-ligand mode can revitalize underutilized ligands, potentially introducing novel and promising chromatographic modes.

Keywords: Adsorption performance; Dual-ligand mode; Hydrophobic charge-induction chromatography; Selectivity factor; Suboptimal ligands.

MeSH terms

Adsorption
Benzimidazoles / chemistry
Chromatography, Liquid / methods
Humans
Hydrogen-Ion Concentration
Hydrophobic and Hydrophilic Interactions*
Immunoglobulin G* / blood
Immunoglobulin G* / chemistry
Ligands
Tryptamines / chemistry

Substances

tryptamine