Multiple Integrated Non-clinical Studies Predict the Safety of Lentivirus-Mediated Gene Therapy for β-Thalassemia

Lidonnici, Maria Rosa; Paleari, Ylenia; Tiboni, Francesca; Mandelli, Giacomo; Rossi, Claudia; Vezzoli, Michela; Aprile, Annamaria; Lederer, Carsten W.; Ambrosi, Alessandro; Chanut, Franck; Sanvito, Francesca; Calabria, Andrea; Poletti, Venerino; Mavilio, Fulvio; Montini, Eugenio; Naldini, Luigi; Cristofori, Patrizia; Ferrari, G.

doi:10.1016/j.omtm.2018.09.001

Cited by 23 publications

(20 citation statements)

References 73 publications

(107 reference statements)

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“…LVV gene therapy has been safe in animal models, [8][9][10][11] and there have been no published cases of insertional oncogenesis in patients thus far. 6,[12][13][14][15] The patient received HU for several years, Cells were collected from the patient at diagnosis (PB), 20 days postdiagnosis of MDS (BM), and 8 days post-AML recurrence (PB and BM).…”

Section: Resultsmentioning

confidence: 99%

Myelodysplastic syndrome unrelated to lentiviral vector in a patient treated with gene therapy for sickle cell disease

et al. 2020

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Section: Resultsmentioning

confidence: 99%

Myelodysplastic syndrome unrelated to lentiviral vector in a patient treated with gene therapy for sickle cell disease

et al. 2020

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“…Additional clinical studies are required to determine whether there are any interactions between the viral vectors and the genome of the patient, and the effects of such interactions. In β-thalassemia gene therapy, due to erythroid-restricted activity of promoters, there is a very low probability of genotoxicity caused by trans-activation (67). Thus, no toxicity or tumor production has been reported in studies where lentiviral vectors were used in mouse models.…”

Section: Gene-based Therapiesmentioning

confidence: 99%

“…Thus, no toxicity or tumor production has been reported in studies where lentiviral vectors were used in mouse models. However, checks are required to ensure the vector has not inserted, the toxicity of the vector and germline transfer (67). A recent study showed that the absence of transplant based mortality as well as replication of competent lentiviruses resulted in other complications, such as febrile neutropenia, epistaxis, stomatitis, pyrexia, irregular menstruation and liver diseases in some patients (68).…”

Section: Gene-based Therapiesmentioning

confidence: 99%

Novel genetic therapeutic approaches for modulating the severity of β‑thalassemia (Review)

et al. 2020

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Thalassemia is a genetic haematological disorder that arises due to defects in the α and β-globin genes. Worldwide, 0.3-0.4 million children are born with haemoglobinopathies per year. Thalassemic patients, as well as their families, face various serious clinical, socioeconomic , and psychosocial challenges throughout their life. Different therapies are available in clinical practice to minimize the suffering of thalassemic patients to some extent and potentially cure the disease. Predominantly, patients undergo transfusion therapy to maintain their haemoglobin levels. Due to multiple transfusions, the iron levels in their bodies are elevated. Iron overload results in damage to body organs, resulting in heart failure, liver function failure or endocrine failure, all of which are commonly observed. Certain drugs have been developed to enhance the expression of the γ-gene, which ultimately results in augmentation of fetal haemoglobin (HbF) levels and total haemoglobin levels in the body. However, its effectiveness is dependent on the genetic makeup of the individual patient. At present, allogeneic haematopoietic Stem Cell Transplantation (HSCT) is the only practically available option with a high curative rate. However, the outcome of HSCT is strongly influenced by factors such as age at transplantation, irregular iron chelation history before transplantation, histocompatibility, and source of stem cells. Gene therapy using the lentiglobin vector is the most recent method for cure without any mortality, graft rejection and clonal dominance issues. However, delayed platelet engraftment is being reported in some patients. Genome editing is a novel approach which may be used to treat patients with thalassemia; it makes use of targeted nucleases to correct the mutations in specific DNA sequences and modify the sequence to the normal wild-type sequence. To edit the genome at the required sites, CRISPR/Cas9 is an efficient and accurate tool that is used in various genetic engineering programs. Genome editing mediated by CRISPR/Cas9 has the ability to restore the normal β-globin function with minimal side effects. Using CRISPR/Cas9, expression of BCL11A can be downregulated along with increased production of HbF. However, these genome editing tools are still under in-vitro trials. CRISPR/Cas9 has can be used for precise transcriptional regulation, genome modification and epigenetic editing. Additional research is required in this regard, as CRISPR/Cas9 may potentially exhibit off-target activity and there are legal and ethical considerations regarding its use. Contents 1. Introduction 2. Therapeutic options for thalassemia 3. Gene-based therapies 4. Conclusions

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“…2-3 viralen Vektoren in das Wirtsgenom ist das Risiko einer Onkogenaktivierung damit ausgesprochen geringaber wahrscheinlich auch nicht null. So sind in einer zunehmenden Zahl von klinischen Studien mit lentiviralen Vektoren für die Behandlung unterschiedlicher genetischer Erkrankungen bislang noch keine durch die Integration der Viren verursachte Sekundärleukämien oder andere maligne Erkrankungen beobachtet worden [33,44,45]. Allerdings ist die Anzahl von behandelten Patienten noch klein (< 100) und die Dauer der Nachbeobachtung insgesamt noch kurz, sodass eine abschließende Bewertung des Risikopotenzials dieses Vektortypus heute noch nicht möglich ist.…”

Section: Neue Self-inactivating Lentivirale Vektorenunclassified

Gentherapie von Hämoglobinkrankheiten – aktuelle Konzepte und Herausforderungen

Kulozik

Kunz

2019

Transfusionsmedizin

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ZusammenfassungDie β-Thalassämien und die Sichelzellerkrankung sind weltweit die häufigsten Einzelgendefekte, die konventionell nur durch eine lebenslang erforderliche Supportivtherapie oder kurativ mittels allogener Stammzelltransplantation behandelbar sind. Aktuell werden Gentherapiestrategien entwickelt, die nach Transduktion von hämatopoetischen Stammzellen durch lentivirale Vektoren zu einer Expression eines therapeutischen β-Globin-Gens oder zur therapeutischen Reexpression der fetalen Globinsynthese und damit des fetalen Hämoglobins (HbF) führen. Für die β-Thalassämie hat die Genadditionstherapie für eine ausgewählte Gruppe von Patientinnen und Patienten mit transfusionsbedürftiger Non-β0-Thalassaemia major nach konditionaler Zulassung durch die European Medicines Agency (EMA) im Juni 2019 einen ersten Grad klinischer Reife erreicht. In dieser Übersicht diskutieren wir darüber hinaus die Möglichkeiten und Herausforderungen von Genomeditierungsstrategien für die Hämoglobinkrankheiten, insbesondere durch Inaktivierung von BCL11A, des zentralen Inhibitors der postnatalen fetalen Hämoglobinsynthese. Insgesamt verspricht die Entwicklung der Gentherapie für die Hämoglobinkrankheiten eine relevante Chance für diese, auch in Deutschland zahlreicher werdenden Gruppe von Patientinnen und Patienten mit schweren, sowohl Lebensqualität als auch Lebenserwartung erheblich einschränkenden Erkrankungen.

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Multiple Integrated Non-clinical Studies Predict the Safety of Lentivirus-Mediated Gene Therapy for β-Thalassemia

Cited by 23 publications

References 73 publications

Myelodysplastic syndrome unrelated to lentiviral vector in a patient treated with gene therapy for sickle cell disease

Myelodysplastic syndrome unrelated to lentiviral vector in a patient treated with gene therapy for sickle cell disease

Novel genetic therapeutic approaches for modulating the severity of β‑thalassemia (Review)

Gentherapie von Hämoglobinkrankheiten – aktuelle Konzepte und Herausforderungen

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Multiple Integrated Non-clinical Studies Predict the Safety of Lentivirus-Mediated Gene Therapy for β-Thalassemia

Cited by 23 publications

References 73 publications

Myelodysplastic syndrome unrelated to lentiviral vector in a patient treated with gene therapy for sickle cell disease

Myelodysplastic syndrome unrelated to lentiviral vector in a patient treated with gene therapy for sickle cell disease

Novel genetic therapeutic approaches for modulating the severity of &beta;‑thalassemia (Review)

Gentherapie von Hämoglobinkrankheiten – aktuelle Konzepte und Herausforderungen

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Novel genetic therapeutic approaches for modulating the severity of β‑thalassemia (Review)