Culture temperature modulates half antibody and aggregate formation in a Chinese hamster ovary cell line expressing a bispecific antibody

Gómez, Natalia; Wieczorek, Agatha; Lu, Fang; Bruno, Richele; Díaz, Luis A.; Agrawal, Neeraj J.; Daris, Kristi

doi:10.1002/bit.26803

Cited by 12 publications

(10 citation statements)

References 30 publications

(46 reference statements)

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“…Indeed, for in vivo assembly, the efficient co-expression of engineered heavy and light chains relies deeply on the selection of stably expressing cell clones. Plus, culture conditions such as temperature also affect the half-antibody expression and aggregate formation [184]. In contrast, following downstream Protein A purification of CH3 mutants, in vitro assembly (separate expression of two different heavy-chain types followed by mixing them at appropriate redox conditions to induce assembly) have demonstrated their capability in generating high-quality molecules.…”

Section: Strategies To Improve Bispecific Antibody Production and mentioning

confidence: 99%

Design and Production of Bispecific Antibodies

et al. 2019

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With the current biotherapeutic market dominated by antibody molecules, bispecific antibodies represent a key component of the next-generation of antibody therapy. Bispecific antibodies can target two different antigens at the same time, such as simultaneously binding tumor cell receptors and recruiting cytotoxic immune cells. Structural diversity has been fast-growing in the bispecific antibody field, creating a plethora of novel bispecific antibody scaffolds, which provide great functional variety. Two common formats of bispecific antibodies on the market are the single-chain variable fragment (scFv)-based (no Fc fragment) antibody and the full-length IgG-like asymmetric antibody. Unlike the conventional monoclonal antibodies, great production challenges with respect to the quantity, quality, and stability of bispecific antibodies have hampered their wider clinical application and acceptance. In this review, we focus on these two major bispecific types and describe recent advances in the design, production, and quality of these molecules, which will enable this important class of biologics to reach their therapeutic potential.

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Section: Strategies To Improve Bispecific Antibody Production and mentioning

confidence: 99%

Design and Production of Bispecific Antibodies

et al. 2019

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“…Although heat shock protein 70 (HSP70) can delay the expression of caspase-3, increase the lifespan of the cells, and protect the cells, it can arrest the G2/M phase cell cycle, which occurs at a temperature no higher than the optimal cell culture temperature. It is also conducive to the production of mAbs [32][33] . When the culture temperature is lower than the optimal temperature, cell viability and lifespan are also affected.…”

Section: Temperaturementioning

confidence: 99%

Research Update on Bioreactors Used in Tissue Engineering

Wang

Deng

et al. 2021

J. Shanghai Jiaotong Univ. (Sci.)

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Owing to the paucity of donor organs and their acute rejection by the immune system after transplantation, advanced organ failure is one of the major challenges faced by the medical community. Static culturing used for synthesising tissues and organs cannot simulate the in vivo mechanical and biochemical signals; therefore, such artificial organs fail to maintain effective functional activity following transplantation. Tissue engineering can overcome these hurdles by successfully enabling regeneration of tissues and organs in vitro. Bioreactors are pivotal in the development and generation of engineered biological products. They simulate the in vivo microenvironment of tissue growth while also providing various mechanical stimuli and biochemical signals to stem cells to effectively generate transplantable organs or tissues. Various designs and types of bioreactors, their applications, and future research prospects are summarised, which promote functional tissue engineering.

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“…A bispecific antibody has two different light chains and two different heavy chains pair via engineered interchain interactions. Furthermore, bispecific antibodies have high efficacy for cytotoxicity, high affinity and small in size (easily penetrable to tissues) [64][65].…”

Section: Naked Antibodies Bispecific Antibodies and Conjugated Antibmentioning

confidence: 99%

Development of Therapeutic Antibody Technology And Recent Perspectives For Leukemia-Lymphoma Treatment

Yirga¹,

Lin²,

Huang³

et al. 2019

J Leuk

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Advancement of monoclonal antibodies (Mabs) to be accepted as a therapy has long history. This article describes the dramatic developmental trend of therapeutic antibody technology and their significant role for treatment of leukemia-lymphoma at the current time. The therapeutic Mab technology development from murine (mouse origin) to fully human resulted in low immunogenicity and high quality Mabs. Chemotherapy is standard care for leukemialymphoma treatments. However, it is associated with high toxicities (side effects), painful and relatively ineffective against certain leukemia-lymphoma subtypes. The remarkable contribution of Von Behring, Paul Ehrlich and the discovery of hybridoma technology marked the beginning of antibodies for therapeutic applications. Rituximab is the first Mab approved by Food and Drug Administration against B-cell malignancies. Today, a number of effective Mabs targeting leukemia and lymphoma were approved and successfully developed. The Mab therapeutic phenomena in the body (also called war in the blood) has various mechanism of actions. In recent years, Mab against leukemialymphoma achieved significantly therapeutic outcomes, eventually this led to traditional chemotherapy treatment free era. We also reviewed that, the therapeutic efficacy of Mabs against leukemia-lymphoma as compared antibody alone and antibody conjugated with potent chemotherapy or cytotoxic drugs. This article extends our understanding of advancements in therapeutic Mabs technology and provides new insights of Mab leukemia-lymphomas therapy. We also encourage further more studies for Mab based diagnostics, treatments of leukemia and lymphomas.

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Culture temperature modulates half antibody and aggregate formation in a Chinese hamster ovary cell line expressing a bispecific antibody

Cited by 12 publications

References 30 publications

Design and Production of Bispecific Antibodies

Design and Production of Bispecific Antibodies

Research Update on Bioreactors Used in Tissue Engineering

Development of Therapeutic Antibody Technology And Recent Perspectives For Leukemia-Lymphoma Treatment

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