DOAJ Open Access 2022

Autologous, lentivirus‐modified, T‐rapa cell “micropharmacies” for lysosomal storage disorders

Murtaza S Nagree Tania C Felizardo Mary L Faber Jitka Rybova C Anthony Rupar +4 lainnya

Abstrak

Abstract T cells are the current choice for many cell therapy applications. They are relatively easy to access, expand in culture, and genetically modify. Rapamycin‐conditioning ex vivo reprograms T cells, increasing their memory properties and capacity for survival, while reducing inflammatory potential and the amount of preparative conditioning required for engraftment. Rapamycin‐conditioned T cells have been tested in patients and deemed to be safe to administer in numerous settings, with reduced occurrence of infusion‐related adverse events. We demonstrate that ex vivo lentivirus‐modified, rapamycin‐conditioned CD4+ T cells can also act as next‐generation cellular delivery vehicles—that is, “micropharmacies”—to disseminate corrective enzymes for multiple lysosomal storage disorders. We evaluated the therapeutic potential of this treatment platform for Fabry, Gaucher, Farber, and Pompe diseases in vitro and in vivo. For example, such micropharmacies expressing α‐galactosidase A for treatment of Fabry disease were transplanted in mice where they provided functional enzyme in key affected tissues such as kidney and heart, facilitating clearance of pathogenic substrate after a single administration.

Penulis (9)

M

Murtaza S Nagree

T

Tania C Felizardo

M

Mary L Faber

J

Jitka Rybova

C

C Anthony Rupar

S

S Ronan Foley

M

Maria Fuller

D

Daniel H Fowler

J

Jeffrey A Medin

Format Sitasi

Nagree, M.S., Felizardo, T.C., Faber, M.L., Rybova, J., Rupar, C.A., Foley, S.R. et al. (2022). Autologous, lentivirus‐modified, T‐rapa cell “micropharmacies” for lysosomal storage disorders. https://doi.org/10.15252/emmm.202114297

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Informasi Jurnal
Tahun Terbit
2022
Sumber Database
DOAJ
DOI
10.15252/emmm.202114297
Akses
Open Access ✓