Biotherapeutics

Mammalian Chinese hamster ovary (CHO) cells dominate therapeutic protein production thanks to their ability to perform human-like post-translational modifications, while microbial hosts such as E. coli and yeast are used for simpler proteins, peptides and viral vector components.

A therapeutic IgG antibody is built from two heavy and two light chains forming a Y-shaped molecule with two antigen-binding (Fab) regions and one effector-function (Fc) region. The Fab arms determine target specificity, while the Fc region governs immune mechanisms such as antibody-dependent cellular cytotoxicity (ADCC) and complement-dependent cytotoxicity (CDC).

IgG antibodies carry a conserved N-glycan at asparagine 297 (Asn297) in the Fc region. Its composition directly modulates Fcγ-receptor binding, ADCC potency, thermal stability, half-life and immunogenicity — making glycan profile control one of the central goals of bioprocess development.

Productivity and product quality are governed by cellular parameters such as viable cell density, specific productivity and metabolic state. Bioreactor parameters — temperature, pH, dissolved oxygen, agitation and feeding strategy — are tuned to keep cells in their optimal physiological window. 

Coupling a perfused N-1 seed bioreactor with a high-inoculation-density production stage delivers reported titer increases of approximately 85% and space–time yield gains over 130% in CHO-based mAb production.

Alternating tangential flow (ATF) and acoustic cell retention enable culture durations of weeks to months at very high cell densities, maintaining cells in a steady physiological state and improving product consistency.

Pre-sterilised single-use bioreactors reduce cleaning validation, shorten changeover and lower contamination risk, and have become a default for clinical-scale mAb, viral vector and vaccine production.

CRISPR-Cas9-based gene editing and AI-supported bioprocess modelling enable tailored production hosts and predictive process control, accelerating the path from clone selection to clinical manufacturing.

Cell line productivity and long-term phenotypic stability; consistent control of post-translational modifications such as glycosylation; bioprocess heterogeneity caused by gradients in dissolved oxygen, pH and shear during scale-up; and downstream bottlenecks created by intensified upstream titers.

Continuous and intensified bioprocesses — particularly N-1 perfusion and fully continuous upstream operations — are expected to become the new standard, supported by perfusion-adapted cell lines and advanced cell retention technology. Glycoengineering, synthetic biology and CRISPR-based host cell design enable tailored production cells with optimised metabolism, while AI-driven bioprocess modelling accelerates the timeline from discovery to clinical manufacturing.