Zellweger Spectrum Disorder

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This entry is adapted from the peer-reviewed paper https://medlineplus.gov/genetics/condition/zellweger-spectrum-disorder

Zellweger spectrum disorder is a group of conditions that have overlapping signs and symptoms and affect many parts of the body.

genetic conditions

1. Introduction

This group of conditions includes Zellweger syndrome, neonatal adrenoleukodystrophy (NALD), and infantile Refsum disease. These conditions were once thought to be distinct disorders but are now considered to be part of the same condition spectrum. Zellweger syndrome is the most severe form of the Zellweger spectrum disorder, NALD is intermediate in severity, and infantile Refsum disease is the least severe form. Because these three conditions are now considered one disorder, some researchers prefer not to use the separate condition names but to instead refer to cases as severe, intermediate, or mild.

Individuals with Zellweger syndrome, at the severe end of the spectrum, develop signs and symptoms of the condition during the newborn period. These infants experience weak muscle tone (hypotonia), feeding problems, hearing and vision loss, and seizures. These problems are caused by the breakdown of myelin, which is the covering that protects nerves and promotes the efficient transmission of nerve impulses. The part of the brain and spinal cord that contains myelin is called white matter. Destruction of myelin (demyelination) leads to loss of white matter (leukodystrophy). Children with Zellweger syndrome also develop life-threatening problems in other organs and tissues, such as the liver, heart, and kidneys. They may have skeletal abnormalities, including a large space between the bones of the skull (fontanelles) and characteristic bone spots known as chondrodysplasia punctata that can be seen on x-ray. Affected individuals have distinctive facial features, including a flattened face, broad nasal bridge, and high forehead. Children with Zellweger syndrome typically do not survive beyond the first year of life.

People with NALD or infantile Refsum disease, which are at the less-severe end of the spectrum, have more variable features than those with Zellweger syndrome and usually do not develop signs and symptoms of the disease until late infancy or early childhood. They may have many of the features of Zellweger syndrome; however, their condition typically progresses more slowly. Children with these less-severe conditions often have hypotonia, vision problems, hearing loss, liver dysfunction, developmental delay, and some degree of intellectual disability. Most people with NALD survive into childhood, and those with infantile Refsum disease may reach adulthood. In rare cases, individuals at the mildest end of the condition spectrum have developmental delay in childhood and hearing loss or vision problems beginning in adulthood and do not develop the other features of this disorder.

2. Frequency

Zellweger spectrum disorder is estimated to occur in 1 in 50,000 individuals.

3. Causes

Mutations in at least 12 genes have been found to cause Zellweger spectrum disorder. These genes provide instructions for making a group of proteins known as peroxins, which are essential for the formation and normal functioning of cell structures called peroxisomes. Peroxisomes are sac-like compartments that contain enzymes needed to break down many different substances, including fatty acids and certain toxic compounds. They are also important for the production of fats (lipids) used in digestion and in the nervous system. Peroxins assist in the formation (biogenesis) of peroxisomes by producing the membrane that separates the peroxisome from the rest of the cell and by importing enzymes into the peroxisome.

Mutations in the genes that cause Zellweger spectrum disorder prevent peroxisomes from forming normally. Diseases that disrupt the formation of peroxisomes, including Zellweger spectrum disorder, are called peroxisome biogenesis disorders. If the production of peroxisomes is altered, these structures cannot perform their usual functions. The signs and symptoms of Zellweger syndrome are due to the absence of functional peroxisomes within cells. NALD and infantile Refsum disease are caused by mutations that allow some peroxisomes to form.

Mutations in the PEX1 gene are the most common cause of Zellweger spectrum disorder and are found in nearly 70 percent of affected individuals. The other genes associated with Zellweger spectrum disorder each account for a smaller percentage of cases of this condition.

4. Inheritance

This condition is inherited in an autosomal recessive pattern, which means both copies of the gene in each cell have mutations. The parents of an individual with an autosomal recessive condition each carry one copy of the mutated gene, but they typically do not show signs and symptoms of the condition.

5. aOther Names for This Condition

cerebrohepatorenal syndrome
PBD, ZSS
PBD-ZSD
peroxisome biogenesis disorders, Zellweger syndrome spectrum
Zellweger spectrum
Zellweger syndrome spectrum
ZSD

References

Braverman NE, D'Agostino MD, Maclean GE. Peroxisome biogenesis disorders:Biological, clinical and pathophysiological perspectives. Dev Disabil Res Rev.2013;17(3):187-96. doi: 10.1002/ddrr.1113. Review.
Crane DI, Maxwell MA, Paton BC. PEX1 mutations in the Zellweger spectrum ofthe peroxisome biogenesis disorders. Hum Mutat. 2005 Sep;26(3):167-75. Review.
Ebberink MS, Koster J, Visser G, Spronsen Fv, Stolte-Dijkstra I, Smit GP, FockJM, Kemp S, Wanders RJ, Waterham HR. A novel defect of peroxisome division due toa homozygous non-sense mutation in the PEX11β gene. J Med Genet. 2012May;49(5):307-13. doi: 10.1136/jmedgenet-2012-100778.
Ebberink MS, Mooijer PA, Gootjes J, Koster J, Wanders RJ, Waterham HR. Geneticclassification and mutational spectrum of more than 600 patients with a Zellwegersyndrome spectrum disorder. Hum Mutat. 2011 Jan;32(1):59-69. doi:10.1002/humu.21388.
Rosewich H, Ohlenbusch A, Gärtner J. Genetic and clinical aspects of Zellwegerspectrum patients with PEX1 mutations. J Med Genet. 2005 Sep;42(9):e58.
Steinberg SJ, Dodt G, Raymond GV, Braverman NE, Moser AB, Moser HW. Peroxisomebiogenesis disorders. Biochim Biophys Acta. 2006 Dec;1763(12):1733-48.
Steinberg SJ, Raymond GV, Braverman NE, Moser AB. Zellweger Spectrum Disorder.2003 Dec 12 [updated 2020 Oct 29]. In: Adam MP, Ardinger HH, Pagon RA, WallaceSE, Bean LJH, Stephens K, Amemiya A, editors. GeneReviews® [Internet]. Seattle(WA): University of Washington, Seattle; 1993-2020. Available fromhttp://www.ncbi.nlm.nih.gov/books/NBK1448/
Wanders RJ, Waterham HR. Peroxisomal disorders I: biochemistry and genetics ofperoxisome biogenesis disorders. Clin Genet. 2005 Feb;67(2):107-33. Review.

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Table of Contents

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1. Introduction

2. Frequency

3. Causes

4. Inheritance

5. aOther Names for This Condition

References

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1. Introduction

2. Frequency

3. Causes

3.1 The gene associated with Zellweger spectrum disorder

4. Inheritance

5. aOther Names for This Condition

References