Administration of Cells Engineered to Secrete Fviii-mcoET3 in Prenatal Sheep Recipients Results in Sustained Curative Fviii Plasma Levels for 3 Years after Birth, without Immune or Toxicity-Related Adverse Events

Rodriguez, Martin; Trevisan, Brady; George, Sunil; Ramamurthy, Ritu M; Rabah, Andrew; Shields, Jordan E; Schwahn, Denise J.; Figueroa, Jorge; Meares, Diane; Owen, John; Gautreaux, Michael D.; Atala, Anthony; Doering, Christopher B.; Spencer, H. Trent; Porada, Christopher D.; Almeida-Porada, M. Graca

doi:10.1182/blood-2020-140845

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“…While direct delivery of vectors is promising, the use of cells as vehicles for gene delivery allows for copy number and integration‐site analyses during product development, which would eliminate the possibility of off‐target effects. In utero transplantation of sheep fetuses with human placental cells transduced with an LVV encoding a bioengineered high‐expression FVIII transgene (mcoET3) resulted in curative and sustained plasma levels of FVIII for at least 3 years after treatment, despite the exponential growth of the sheep with no cellular or humoral response to the human cells or to the FVIII transgene, and no evidence of any lentiviral‐related or procedural toxicity in any tissue 69 . Thus, PSCGT has the potential to change the treatment paradigm, providing an early cure for HA and HB, without sensitizing the recipient to the viral capsid or to the cells that deliver the transgene and preclude the development of antibodies against FVIII or FIX protein.…”

Section: Preclinical Data On Pscgtmentioning

confidence: 99%

Prenatal Somatic Cell Gene Therapies: Charting a Path Toward Clinical Applications (Proceedings of the CERSI‐FDA Meeting)

Herzeg

Almeida‐Porada

Charo³

et al. 2022

The Journal of Clinical Pharma

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We are living in a golden age of medicine in which the availability of prenatal diagnosis, fetal therapy, and gene therapy/editing make it theoretically possible to repair almost any defect in the genetic code. Furthermore, the ability to diagnose genetic disorders before birth and the presence of established surgical techniques enable these therapies to be delivered safely to the fetus. Prenatal therapies are generally used in the second or early third trimester for severe, life-threatening disorders for which there is a clear rationale for intervening before birth. While there has been promising work for prenatal gene therapy in preclinical models, the path to a clinical prenatal gene therapy approach is complex. We recently held a conference with the University of California, San Francisco-Stanford Center of Excellence in Regulatory Science and Innovation, researchers, patient advocates, regulatory (members of the Food and Drug Administration), and other stakeholders to review the scientific background and rationale for prenatal somatic cell gene therapy for severe monogenic diseases and initiate a dialogue toward a safe regulatory path for phase 1 clinical trials. This review represents a summary of the considerations and discussions from these conversations.

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Section: Preclinical Data On Pscgtmentioning

confidence: 99%