| Literature DB >> 28217429 |
Kazuki Sawamoto1, Yasuyuki Suzuki2, William G Mackenzie1, Mary C Theroux1, Christian Pizarro1, Hiromasa Yabe3, Kenji E Orii4, Robert W Mason1, Tadao Orii5, Shunji Tomatsu6.
Abstract
INTRODUCTION: Morquio A syndrome is characterized by a unique skeletal dysplasia, leading to short neck and trunk, pectus carinatum, laxity of joints, kyphoscoliosis, and tracheal obstruction. Cervical spinal cord compression/inability, a restrictive and obstructive airway, and/or bone deformity and imbalance of growth, are life-threatening to Morquio A patients, leading to a high morbidity and mortality. It is critical to review the current therapeutic approaches with respect to their efficacy and limitations. AREAS COVERED: Patients with progressive skeletal dysplasia often need to undergo orthopedic surgical interventions in the first two decades of life. Recently, we have treated four patients with a new surgery to correct progressive tracheal obstruction. Enzyme replacement therapy (ERT) has been approved clinically. Cell-based therapies such as hematopoietic stem cell therapy (HSCT) and gene therapy are typically one-time, permanent treatments for enzyme deficiencies. We report here on four Morquio A patients treated with HSCT approved in Japan and followed for at least ten years after treatment. Gene therapy is under investigation on mouse models but not yet available as a therapeutic option. EXPERT OPINION: ERT and HSCT in combination with surgical intervention(s) are a therapeutic option for Morquio A; however, the approach for bone and cartilage lesion remains an unmet challenge.Entities:
Keywords: ERT; HSCT; Morquio A; gene therapy; orthopedic surgery; tracheal obstruction
Year: 2016 PMID: 28217429 PMCID: PMC5312776 DOI: 10.1080/21678707.2016.1214572
Source DB: PubMed Journal: Expert Opin Orphan Drugs ISSN: 2167-8707 Impact factor: 0.694