Resolution of Serious Vaso-Occlusive Pain Crises and Reduction in Patient-Reported Pain Intensity: Results from the Ongoing Phase 1/2 HGB-206 Group C Study of LentiGlobin for Sickle Cell Disease (bb1111) Gene Therapy

Thompson, Alexis A.; Walters, Mark C.; Mapara, Markus Y.; Kwiatkowski, Janet L.; Krishnamurti, Lakshmanan; Aygün, Banu; Kasow, Kimberly A.; Rifkin-Zenenberg, Stacey; Schmidt, Manfred; DelCarpini, Jay; Pierciey, Francis J.; Miller, Alexandra; Gallagher, M.; Ren, Chao; Kanter, Julie; Tisdale, John F.

doi:10.1182/blood-2020-134940

Cited by 9 publications

(20 citation statements)

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“…The BB305 vector contains an additional feature, a codon replacement that causes a tryptophan to glutamine substitution at position 87 in the β-globin protein sequence (T87Q) that interferes with polymerization of HbS tetramers, thus increasing its potential efficacy in the treatment of SCD. A pilot trial using this vector to treat SCD patients provided encouraging results [ 11 ], though a larger trial (NCT0214055) showed variable response and an even stronger requirement for high VCN compared to β-thalassemia [ 79 ].…”

Section: Designing a Transgene Expression Cassettementioning

confidence: 99%

Designing Lentiviral Vectors for Gene Therapy of Genetic Diseases

Poletti

Mavilio

2021

Viruses

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Lentiviral vectors are the most frequently used tool to stably transfer and express genes in the context of gene therapy for monogenic diseases. The vast majority of clinical applications involves an ex vivo modality whereby lentiviral vectors are used to transduce autologous somatic cells, obtained from patients and re-delivered to patients after transduction. Examples are hematopoietic stem cells used in gene therapy for hematological or neurometabolic diseases or T cells for immunotherapy of cancer. We review the design and use of lentiviral vectors in gene therapy of monogenic diseases, with a focus on controlling gene expression by transcriptional or post-transcriptional mechanisms in the context of vectors that have already entered a clinical development phase.

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Section: Designing a Transgene Expression Cassettementioning

confidence: 99%

Designing Lentiviral Vectors for Gene Therapy of Genetic Diseases

Poletti

Mavilio

2021

Viruses

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“…The impact of gene therapy on patient QoL remains to be fully determined and should be further evaluated in future clinical trials of beti-cel. However, data from the phase 3 Hgb-207 (Northstar-2) and Hgb-212 (Northstar-3) studies showed that patients under 18 years of age who achieved transfusion independence had an improved EuroQoL 5 dimensions (Youth) (EQ-5D-Y) score (67 [range 50-96] versus 92.5 [85][86][87][88][89][90][91][92][93][94][95]) after 12 months [67,90]. In addition, HSCT has been shown to have a positive impact on both physical and emotional aspects of HRQoL in patients with TD β-thalassemia and, given GVHD was the most common cause of impaired HRQoL in these patients, a similar or greater benefit would be expected from gene therapy [67].…”

Section: Beti-cel Gene Therapy: Benefits and Challengesmentioning

confidence: 99%

Improving outcomes and quality of life for patients with transfusion-dependent β-thalassemia: recommendations for best clinical practice and the use of novel treatment strategies

Taher

Bou‐Fakhredin

Kattamis

et al. 2021

Expert Review of Hematology

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Introduction: β-thalassemia is one of the most common inherited monogenic diseases. Many patients are dependent on a lifetime of red blood cell (RBC) transfusions and iron chelation therapy. Although treatments have a significant impact on quality of life (QoL), life expectancy, and long-term health outcomes have improved in recent decades through safer RBC transfusion practices and better iron chelation strategies. Advances in the understanding of the pathology of β-thalassemia have led to the development of new treatment options that have the potential to reduce the RBC transfusion burden in patients with transfusion-dependent (TD) β-thalassemia and improve QoL.Areas covered: This review provides an overview of currently available treatments for patients with TD βthalassemia, highlighting QoL issues, and providing an update on current clinical experience plus important practical points for two new treatments available for TD β-thalassemia: betibeglogene autotemcel (beti-cel) gene therapy and the erythroid maturation agent luspatercept, an activin ligand trap. Expert opinion: Approved therapies, including curative gene therapies and supportive treatments such as luspatercept, have the potential to reduce RBC transfusion burden, and improve clinical outcomes and QoL in patients with TD β-thalassemia. Cost of treatment is, however, likely to be a significant barrier for payors and patients.

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“…Haematopoietic stem cell transplantation and gene therapy studies have reported patient Hb levels >100 g/l, with varying percentages of HbS 29–34 . Most patients in HSCT and gene therapy studies had their Hb increase beyond 100 g/l within six to 12 months after transplant.…”

Section: Sickle Cell Disease Therapies and Haemoglobin Elevationmentioning

confidence: 99%

“…Most patients in HSCT and gene therapy studies had their Hb increase beyond 100 g/l within six to 12 months after transplant. Patients also experienced reduction or an absence of VOCs or ACS following transplant in studies that evaluated SCD‐related clinical outcomes 32,34 . Most patients who were receiving chronic transfusion therapy before treatment were able to stop or reduce the frequency of their RBC transfusions within two to three months after gene therapy 31,32,34 .…”

Section: Sickle Cell Disease Therapies and Haemoglobin Elevationmentioning

confidence: 99%

“…For HSCT, post‐transplant complications included sirolimus‐associated complications (pneumonitis, arthralgias), abdominal pain, primary graft failure and graft rejection 29,33 . In gene therapy studies, adverse events were generally associated with the transplantation 31,32,34 . The most common grade ≥3 adverse events included nausea and haematologic alterations associated with myeloablative conditioning 31,32 …”

Section: Sickle Cell Disease Therapies and Haemoglobin Elevationmentioning

confidence: 99%

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Time to rethink haemoglobin threshold guidelines in sickle cell disease

Ballas

Kuypers²,

Hankins

et al. 2021

Br J Haematol

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Summary Alleviating anaemia in patients with sickle cell disease (SCD) is crucial in managing acute complications, mitigating end‐organ damage and preventing early mortality. Some disease‐modifying and curative therapies have increased haemoglobin (Hb) levels to exceed 100 g/l, a threshold above which complications from red blood cell (RBC) transfusions have occurred, raising concern about whole‐blood viscosity‐related complications with these therapies. Here we discuss the rationale behind this limit, the effect of viscosity on blood flow and the applicability of this Hb threshold to therapies for SCD beyond RBC transfusions.

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Resolution of Serious Vaso-Occlusive Pain Crises and Reduction in Patient-Reported Pain Intensity: Results from the Ongoing Phase 1/2 HGB-206 Group C Study of LentiGlobin for Sickle Cell Disease (bb1111) Gene Therapy

Cited by 9 publications

References 0 publications

Designing Lentiviral Vectors for Gene Therapy of Genetic Diseases

Designing Lentiviral Vectors for Gene Therapy of Genetic Diseases

Improving outcomes and quality of life for patients with transfusion-dependent β-thalassemia: recommendations for best clinical practice and the use of novel treatment strategies

Time to rethink haemoglobin threshold guidelines in sickle cell disease

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