The Intrabody Against Murine Double Minute 2 via a p53-Dependent Pathway Induces Apoptosis of Cancer Cell
Changli Wang, Wanting Liu, Haotian Guo, Tian Lan, Tianyi Wang, Bing Wang

TL;DR
A new antibody targeting MDM2 helps activate p53, leading to cancer cell death and reduced tumor growth.
Contribution
A human-derived intrabody (VH-HT3) was developed to inhibit MDM2 and activate p53, showing tumor-suppressive effects.
Findings
VH-HT3 inhibits MDM2 and activates p53, leading to apoptosis in cancer cells.
VH-HT3 induces cell cycle arrest and reduces tumor growth in xenograft models.
VH-HT3 increases HIPK2 levels and activates p53 at the Ser46 site.
Abstract
Murine double minute 2 (MDM2) is involved in various cancers and is an attractive target. The RING domain of MDM2 has been discussed as an alternative target to stabilize p53. Designing drugs to target the RING domain of MDM2 is an alternative approach to preventing MDM2-mediated deactivation of p53. In this study, we obtained a human VH single-domain antibody and revealed its regulatory effects and mechanisms. The RING domain of MDM2 was synthesized using a chemical synthesis method, and antibodies against the MDM2 RING domain were screened from a human VH single-domain antibody library and expressed intracellularly. A nuclear localization sequence was designed to ensure intrabody efficiency. The binding activity of the individually cloned antibodies was detected using ELISA. MTT and flow cytometry assays were used to detect the reactions related to intrabody in vitro. The combination…
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Taxonomy
TopicsCancer-related Molecular Pathways · Cancer Research and Treatments · Ubiquitin and proteasome pathways
