Hypophosphatasia: presentation and response to asfotase alfa Journal Articles

abstract

• UNLABELLED: Hypophosphatasia (HPP) is a rare bone disease with limited scientific evidence on the tolerability and safety of its novel treatment, Asfotase Alfa (AA). We report 7 HPP patients' heterogenous presentations and the significant improvement in various clinical outcomes attained with AA shedding light on this highly effective and safe therapy. INTRODUCTION: Hypophosphatasia (HPP) is a rare inherited metabolic bone disorder characterized by a deficiency in the tissue non-specific alkaline phosphatase (TNSALP) due to loss of function mutation in the ALPL gene. HPP is associated with impaired skeletal mineralization due to elevations in inorganic pyrophosphate and altered phosphate : pyrophosphate ratio. Asfotase alfa (AA) "enzyme replacement" was approved for treatment of HPP in 2015. We present 7 patients with HPP, 5 with pediatric-onset, and 2 with adult-onset, who have been treated with AA and describe the efficacy and safety in these patients. METHODS: 7 patients (4 females, 3 males) aged 19-68 years with HPP were included in this study. Diagnosis of HPP was confirmed by DNA analysis. AA was administered in doses of 6mg/kg/week with a mean follow-up of 6 months (SD= 5). RESULTS: Subjective improvement in muscle strength, muscle pain, walking ability, and walking distance with a reduction in the use of gait aids was seen "with AA in HPP patients." Muscle strength and pain improved by up to 70% from baseline as quantified subjectively by patients. Walking distance improved by up to 100%. Patients also reported improved cognition, mood, and energy levels, with up to 90% improvement in mood and 75% improvement in energy levels. 4 out of 6 patients first noted clinical signs of improvement after 3 months of being on therapy. 1 out of the 7 patients sustained a toe fracture 10 months from being on AA. AA was well-tolerated with injection site reactions being the most reported adverse effect. CONCLUSION: HPP treatment with AA in individuals with both pediatric and adult-onset forms resulted in significant subjective improvement in musculoskeletal and cognitive manifestations in addition to patients' quality of life. The drug was well tolerated in 6 patients. 1 patient discontinued therapy because of minor adverse effects with myalgias.

authors

• Alsarraf, F
• Ali, DS
• Almonaei, K
• Al-Alwani, H
• Khan, Aliya
• Brandi, ML

status

• published 

publication date

• April 2024

has subject area

• 0903 Biomedical Engineering (FoR)
• 1103 Clinical Sciences (FoR)
• 1117 Public Health and Health Services (FoR)
• Adult (MeSH)
• Alkaline Phosphatase (MeSH)
• Bone Diseases, Metabolic (MeSH)
• Child (MeSH)
• Diphosphates (MeSH)
• Endocrinology & Metabolism (Science Metrix)
• Female (MeSH)
• Humans (MeSH)
• Hypophosphatasia (MeSH)
• Immunoglobulin G (MeSH)
• Male (MeSH)
• Pain (MeSH)
• Quality of Life (MeSH)
• Recombinant Fusion Proteins (MeSH)

published in

• Osteoporosis International  Journal

keywords

• Adult
• Alkaline Phosphatase
• Asfotase alfa
• Bone Diseases, Metabolic
• Child
• Diphosphates
• Female
• Humans
• Hypophosphatasia
• Immunoglobulin G
• Male
• Pain
• Presentation
• Quality of Life
• Recombinant Fusion Proteins
• Treatment

Digital Object Identifier (DOI)

• 10.1007/s00198-023-06943-z

PubMed ID

• 37993691

start page

• 717

end page

• 725

volume

• 35

issue

• 4