A Site-Specific MiniAp4–Trastuzumab Conjugate Prevents Brain Metastasis
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Data de publicació
2025-03-03ISSN
1543-8392
Resum
Monoclonal antibodies (mAbs) are changing cancer treatments. However, the presence of the blood–brain barrier (BBB) and the blood–tumor barrier (BTB) limits the use of mAbs to treat brain cancer or brain metastasis. Molecules that hijack endogenous transport mechanisms on the brain endothelium (brain shuttles) have been shown to increase the transport of large molecules and nanoparticles across the BBB. Among these shuttles, protease-resistant peptides such as MiniAp-4 are particularly efficient. Here, we report the synthesis, characterization, and evaluation of site-specific mAb–brainshuttle antibody conjugates (ASC) based on the anti-HER2 mAb trastuzumab (Tz) and four molecules of MiniAp-4. The ASCs preserve the binding and cell cycle arrest capacity of Tz. MiniAp-4 ASC displays enhanced transport across an in vitro BBB cellular model with respect to Tz and Tz conjugated to Angiopep-2, the brain shuttle that has advanced the most in clinical trials. More importantly, evaluation of Tz-MiniAp4 in a murine brain metastasis model demonstrated that the protease-resistant peptide showed preferential transport across the BBB/BTB, displaying a marked therapeutic effect and protecting against metastasis development. The technology described herein could be applied to any antibody of interest to treat central nervous system-related diseases. MiniAp-4 enhances the brain transport of the monoclonal antibody trastuzumab, preventing brain metastasis.
Tipus de document
Article
Versió del document
Versió publicada
Llengua
Anglès
Matèries (CDU)
577 - Bioquímica. Biologia molecular. Biofísica
616 - Patologia. Medicina clínica. Oncologia
Paraules clau
Brain shuttle peptide
Trastuzumab
Brain metastasis
Barrera hematoencefàlica
Metàstasi
Cervell
Pàgines
p.12
Publicat per
American Chemical Society
Publicat a
Molecular Pharmaceutics 2025, 22, 3, 1384–1395
Número de l'acord de la subvenció
info:eu-repo/grantAgreement/MEIC/PN I+D/BIO2016-75327-R
info:eu-repo/grantAgreement/SUR del DEC/SGR/2017SGR0998
info:eu-repo/grantAgreement/MEIC/PN I+D/SAF2017-89643-R
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© American Chemical Society
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