Immunoresponse against the transgene limits hematopoietic engraftment of mice transplanted in utero with virally transduced fetal liver

Alonso-Ferrero, Maria E; Valeri, Antonio; Yáñez, Rosa María Pérez; Navarro, Susana; Garín, Marina I.; Ramı́rez, Juan Carlos; Bueren, Juan A.; Segovia, José C.

doi:10.1038/gt.2010.160

Cited by 3 publications

(1 citation statement)

References 45 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…74 More recently, fetal gene delivery has been shown to induce postnatal immune tolerance to the transgenic protein in sheep receiving AAV6.2-and AAV8-GFP 75 and macaques receiving AAV5-factor X. 76 Interestingly, there have been publications reporting immune response following fetal gene delivery of vector in mice, 77 gene-modified hematopoietic stem cells in mice 78 and vector delivery in rats, 79 sheep, 80 and monkeys. 81 Possible explanations may be that certain gene products are less tolerogenic than others (considering that most genes in preclinical experiments are human and not conspecific to the preclinical model) and that some modes of delivery may be more tolerogenic or less pro-inflammatory.…”

Section: Fetal Immune Systemmentioning

confidence: 99%

Fetal gene therapy

Waddington

Peranteau

Rahim

et al. 2023

J of Inher Metab Disea

View full text Add to dashboard Cite

Fetal gene therapy was first proposed toward the end of the 1990s when the field of gene therapy was, to quote the Gartner hype cycle, at its “peak of inflated expectations.” Gene therapy was still an immature field but over the ensuing decade, it matured and is now a clinical and market reality. The trajectory of treatment for several genetic diseases is toward earlier intervention. The ability, capacity, and the will to diagnose genetic disease early—in utero—improves day by day. A confluence of clinical trials now signposts a trajectory toward fetal gene therapy. In this review, we recount the history of fetal gene therapy in the context of the broader field, discuss advances in fetal surgery and diagnosis, and explore the full ambit of preclinical gene therapy for inherited metabolic disease.

show abstract

Section: Fetal Immune Systemmentioning

confidence: 99%

Fetal gene therapy

Waddington

Peranteau

Rahim

et al. 2023

J of Inher Metab Disea

View full text Add to dashboard Cite

show abstract

Partial rescue of mucopolysaccharidosis type VII mice with a lifelong engraftment of allogeneic stem cells in utero

Ihara

Umezawa

Onami

et al. 2015

Congenital Anomalies

View full text Add to dashboard Cite

In utero hematopoietic cell transplantation (IUHCT) has been performed in Mucopolysaccharidosis Type VII (MPSVII) mice, but a lifelong engraftment of allogeneic donor cells has not been achieved. In this study, we sought to confirm a lifelong engraftment of allogeneic donor cells immunologically matched to the mother and to achieve partial rescue of phenotypes in the original MPSVII strain through IUHCT by intravenous injection. We performed in vitro fertilization in a MPSVII murine model and transferred affected embryos to ICR/B6-GFP surrogate mothers in cases where fetuses receiving IUHCT were all homozygous. Lineage-depleted cells from ICR/B6-GFP mice were injected intravenously at E14.5. Chimerism was confirmed by flow cytometry at 4 weeks after birth, and β-glucuronidase activity in serum and several phenotypes were assessed at 8 weeks of age or later. Donor cells in chimeric mice from ICR/B6-GFP mothers were detected at death, and were confirmed in several tissues including the brains of sacrificed chimeric mice. Although the serum enzyme activity of chimeric mice was extremely low, the engraftment rate of donor cells correlated with enzyme activity. Furthermore, improvement of bone structure and rescue of reproductive ability were confirmed in our limited preclinical study. We confirmed the lifelong engraftment of donor cells in an original immunocompetent MPSVII murine model using intravenous IUHCT with cells immunologically matched to the mother without myeloablation, and the improvement of several phenotypes.

show abstract