↓ Skip to main content
What is this page? Embed badge

JIMD Reports, Volume 22

Overview of attention for book
Cover of 'JIMD Reports, Volume 22'

Table of Contents

  1. Altmetric Badge
    Book Overview
  2. Altmetric Badge
    Chapter 371 Innate and Adaptive Immune Response in Fabry Disease.
  3. Altmetric Badge
    Chapter 405 Asparagine Synthetase Deficiency: New Inborn Errors of Metabolism
  4. Altmetric Badge
    Chapter 406 Occurrence of Malignant Tumours in the Acute Hepatic Porphyrias.
  5. Altmetric Badge
    Chapter 407 Improvement in Bone Mineral Density and Architecture in a Patient with Gaucher Disease Using Teriparatide
  6. Altmetric Badge
    Chapter 408 Networking Across Borders for Individuals with Organic Acidurias and Urea Cycle Disorders: The E-IMD Consortium
  7. Altmetric Badge
    Chapter 409 Two Novel Mutations in the SLC25A4 Gene in a Patient with Mitochondrial Myopathy
  8. Altmetric Badge
    Chapter 410 Combined Sepiapterin Reductase and Methylmalonyl-CoA Epimerase Deficiency in a Second Patient: Cerebrospinal Fluid Polyunsaturated Fatty Acid Level and Follow-Up Under l -DOPA, 5-HTP and BH4 Trials
  9. Altmetric Badge
    Chapter 411 Audit of the Use of Regular Haem Arginate Infusions in Patients with Acute Porphyria to Prevent Recurrent Symptoms
  10. Altmetric Badge
    Chapter 413 Normal Cerebrospinal Fluid Pyridoxal 5′-Phosphate Level in a PNPO-Deficient Patient with Neonatal-Onset Epileptic Encephalopathy
  11. Altmetric Badge
    Chapter 414 Bladder and Bowel Dysfunction Is Common in Both Men and Women with Mutation of the ABCD1 Gene for X-Linked Adrenoleukodystrophy
  12. Altmetric Badge
    Chapter 415 Extreme Contrast of Postprandial Remnant-Like Particles Formed in Abetalipoproteinemia and Homozygous Familial Hypobetalipoproteinemia.
  13. Altmetric Badge
    Chapter 416 Girls with Seizures Due to the c.320A>G Variant in ALG13 Do Not Show Abnormal Glycosylation Pattern on Standard Testing.
  14. Altmetric Badge
    Chapter 417 Monitoring of Therapy for Mucopolysaccharidosis Type I Using Dysmorphometric Facial Phenotypic Signatures
  15. Altmetric Badge
    Chapter 418 Age at First Cardiac Symptoms in Fabry Disease: Association with a Chinese Hotspot Fabry Mutation (IVS4+919G>A), Classical Fabry Mutations, and Sex in a Taiwanese Population from the Fabry Outcome Survey (FOS)
  16. Altmetric Badge
    Chapter 419 Mitochondrial Complex III Deficiency Caused by TTC19 Defects: Report of a Novel Mutation and Review of Literature.
Attention for Chapter 371: Innate and Adaptive Immune Response in Fabry Disease.
Altmetric Badge

Citations

dimensions_citation
4 Dimensions

Readers on

mendeley
67 Mendeley
Summary Dimensions citations
You are seeing a free-to-access but limited selection of the activity Altmetric has collected about this research output. Click here to find out more.
Chapter title
Innate and Adaptive Immune Response in Fabry Disease.
Chapter number 371
Book title
JIMD Reports, Volume 22
Published in
JIMD Reports, February 2015
DOI 10.1007/8904_2014_371
Pubmed ID
25690728
Book ISBNs
978-3-66-247452-5, 978-3-66-247453-2
Authors

Wladimir Mauhin, Olivier Lidove, Elisa Masat, Federico Mingozzi, Kuberaka Mariampillai, Jean-Marc Ziza, Olivier Benveniste, Mauhin, Wladimir, Lidove, Olivier, Masat, Elisa, Mingozzi, Federico, Mariampillai, Kuberaka, Ziza, Jean-Marc, Benveniste, Olivier

Abstract

Fabry disease is an X-linked lysosomal storage disease in which mutations of the gene (GLA) cause a deficiency of the lysosomal hydrolase α-galactosidase A (α-Gal). This defect results in an accumulation of glycosphingolipids, primarily globotriaosylceramide (Gb3) which causes a multisystemic vasculopathy. Available since 2001 in Europe, enzyme replacement therapy consists in the administration of agalsidase, a recombinant form of α-galactosidase A. Enzyme replacement therapy was shown to improve the global prognosis but allowed partial success in preventing critical events such as strokes and cardiac arrests. As in most lysosomal storage diseases, frequent immune reactions have been described in naive Fabry disease patients. Humoral immune responses following enzyme replacement therapy have also been described, with unclear consequences on the progression of the disease. While cost-effectiveness of enzyme replacement therapy in Fabry disease begins to be questioned and new therapeutic strategies arise such as chaperone or gene therapy, it appears necessary to better understand the immune responses observed in the treatment of naive patients and during enzyme replacement therapy with agalsidase. We propose a comprehensive review of the available literature concerning both innate and adaptive responses observed in Fabry disease. We particularly highlight the probable role of the toll-like receptor 4 (TLR4) and CD1d pathways triggered by Gb3 accumulation in the development of local and systemic inflammation that could lead to irreversible organ damages. We propose an immunological point of view of Fabry disease pathogenesis involving immune cells notably the invariant natural killer T cells. We finally review anti-agalsidase antibodies, their development and impact on outcomes.

View on publisher site
Mendeley readers

Mendeley readers

The data shown below were compiled from readership statistics for 67 Mendeley readers of this research output. Click here to see the associated Mendeley record.

Geographical breakdown

Country Count As %
Unknown 67 100%

Demographic breakdown

Readers by professional status Count As %
Student > Master 10 15%
Student > Bachelor 7 10%
Student > Doctoral Student 6 9%
Researcher 6 9%
Other 4 6%
Other 8 12%
Unknown 26 39%
Readers by discipline Count As %
Medicine and Dentistry 13 19%
Agricultural and Biological Sciences 10 15%
Biochemistry, Genetics and Molecular Biology 4 6%
Immunology and Microbiology 3 4%
Nursing and Health Professions 2 3%
Other 7 10%
Unknown 28 42%

This page is provided by Altmetric.