Bone manifestations in neuronopathic Gaucher disease while receiving high-dose enzyme replacement therapy

Bone manifestations in neuronopathic Gaucher disease while receiving high-dose enzyme replacement therapy

Avascular necrosis (AVN), one type of bone infarction, is a major irreversible complication of Gaucher disease (GD). In this report, two pediatric patients with GD type 3, homozygous for the L483P pathogenic variant (formerly L444P), developed AVN despite treatment on long-term, high-dose enzyme rep...

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Veröffentlicht in:Molecular genetics and metabolism 2019-02, Vol.126 (2), p.157-161
Hauptverfasser: Potnis, Kunal C., Flueckinger, Lauren B., Ha, Christine I., Upadia, Jariya, Frush, Donald P., Kishnani, Priya S.
Format: Artikel
Sprache:eng
Schlagworte:
ACE
Adolescent
Aftercare
angiotensin-converting enzyme
Avascular necrosis
AVN
BMD
Bone and Bones - drug effects
Bone and Bones - pathology
Bone manifestations
bone mineral density
Child
Child, Preschool
CHITO
chitotriosidase
dual-energy X-ray absorptiometry
DXA
Enzyme replacement therapy
Enzyme Replacement Therapy - adverse effects
ERT
Gaucher disease
Gaucher Disease - complications
Gaucher Disease - drug therapy
Humans
Infant
Kyphosis - etiology
magnetic resonance imaging
Male
MRI
Osteonecrosis
Osteonecrosis - etiology
SRT
substrate reduction therapy
tartrate-resistant acid phosphatase
TRAP
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container_end_page 161
container_issue 2
container_start_page 157
container_title Molecular genetics and metabolism
container_volume 126
creator Potnis, Kunal C.
Flueckinger, Lauren B.
Ha, Christine I.
Upadia, Jariya
Frush, Donald P.
Kishnani, Priya S.
description Avascular necrosis (AVN), one type of bone infarction, is a major irreversible complication of Gaucher disease (GD). In this report, two pediatric patients with GD type 3, homozygous for the L483P pathogenic variant (formerly L444P), developed AVN despite treatment on long-term, high-dose enzyme replacement therapy (ERT). ERT was initiated in both patients, who had intact spleens, shortly after diagnosis with an initial dramatic response. However, both patients exhibited AVN after 5.5 and 11 years on high-dose ERT, respectively, despite good compliance and normalized hematological findings and visceral symptoms. This report demonstrates the importance of careful, regular surveillance of the musculoskeletal system in addition to monitoring the neurological symptoms associated with neuronopathic GD. Additionally, it highlights the limitations of ERT in terms of targeting certain sanctuary sites such as bone marrow and suggests the need for new treatment modalities other than ERT monotherapy to address these limitations.
doi_str_mv 10.1016/j.ymgme.2018.11.004
format Article
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In this report, two pediatric patients with GD type 3, homozygous for the L483P pathogenic variant (formerly L444P), developed AVN despite treatment on long-term, high-dose enzyme replacement therapy (ERT). ERT was initiated in both patients, who had intact spleens, shortly after diagnosis with an initial dramatic response. However, both patients exhibited AVN after 5.5 and 11 years on high-dose ERT, respectively, despite good compliance and normalized hematological findings and visceral symptoms. This report demonstrates the importance of careful, regular surveillance of the musculoskeletal system in addition to monitoring the neurological symptoms associated with neuronopathic GD. 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In this report, two pediatric patients with GD type 3, homozygous for the L483P pathogenic variant (formerly L444P), developed AVN despite treatment on long-term, high-dose enzyme replacement therapy (ERT). ERT was initiated in both patients, who had intact spleens, shortly after diagnosis with an initial dramatic response. However, both patients exhibited AVN after 5.5 and 11 years on high-dose ERT, respectively, despite good compliance and normalized hematological findings and visceral symptoms. This report demonstrates the importance of careful, regular surveillance of the musculoskeletal system in addition to monitoring the neurological symptoms associated with neuronopathic GD. 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source MEDLINE; Elsevier ScienceDirect Journals
subjects ACE
Adolescent
Aftercare
angiotensin-converting enzyme
Avascular necrosis
AVN
BMD
Bone and Bones - drug effects
Bone and Bones - pathology
Bone manifestations
bone mineral density
Child
Child, Preschool
CHITO
chitotriosidase
dual-energy X-ray absorptiometry
DXA
Enzyme replacement therapy
Enzyme Replacement Therapy - adverse effects
ERT
Gaucher disease
Gaucher Disease - complications
Gaucher Disease - drug therapy
Humans
Infant
Kyphosis - etiology
magnetic resonance imaging
Male
MRI
Osteonecrosis
Osteonecrosis - etiology
SRT
substrate reduction therapy
tartrate-resistant acid phosphatase
TRAP
title Bone manifestations in neuronopathic Gaucher disease while receiving high-dose enzyme replacement therapy
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