Lysosomal storage disease

Lysosomal storage disease
Classification and external resources
Micrograph of Gaucher disease, with cells that have the characteristic crumpled tissue paper-like cytoplasm. H&E stain.
ICD-10	E 75-E 77
MeSH	D016464

Lysosomal storage diseases (LSDs; /ˌlaɪsəˈsoʊməl/) are a group of approximately 50 rare inherited metabolic disorders that result from defects in lysosomal function.^[1] Lysosomal storage diseases result when a specific organelle in the body's cells – the lysosome – malfunctions.

Lysosomal storage disorders are caused by lysosomal dysfunction usually as a consequence of deficiency of a single enzyme required for the metabolism of lipids, glycoproteins (sugar containing proteins) or so-called mucopolysaccharides. Individually, LSDs occur with incidences of less than 1:100,000; however, as a group the incidence is about 1:5,000 - 1:10,000. Most of these disorders are autosomal recessively inherited such as Niemann-Pick disease, type C, however a few are X-linked recessively inherited, such as Fabry disease and Hunter syndrome (MPS II).

The lysosome is commonly referred to as the cell’s recycling center because it processes unwanted material into substances that the cell can utilize. Lysosomes break down this unwanted matter via enzymes, highly specialized proteins essential for survival. Lysosomal disorders are triggered when a particular enzyme exists in too small an amount or is missing altogether. When this happens, substances accumulate in the cell. In other words, when the lysosome doesn’t function normally, excess products destined for breakdown and recycling are stored in the cell.

Like other genetic diseases, individuals inherit lysosomal storage diseases from their parents. Although each disorder results from different gene mutations that translate into a deficiency in enzyme activity, they all share a common biochemical characteristic – all lysosomal disorders originate from an abnormal accumulation of substances inside the lysosome.

Lysosomal storage diseases affect mostly children and they often die at a young and unpredictable age, many within a few months or years of birth. Many other children die of this disease following years of suffering from various symptoms of their particular disorder.

1 Symptoms
2 Diagnosis
3 Treatment
4 History
5 Classification
6 See also
7 References
8 External links

Symptoms

The symptoms of lysosomal storage disease vary, depending on the particular disorder and other variables like the age of onset, and can be mild to severe. They can include developmental delay, movement disorders, seizures, dementia, deafness and/or blindness. Some people with Lysosomal storage disease have enlarged livers (hepatomegaly) and enlarged spleens (splenomegaly), pulmonary and cardiac problems, and bones that grow abnormally.

Diagnosis

The majority of patients are initially screened by enzyme assay, which is the most efficient method to arrive at a definitive diagnosis. In some families where the disease-causing mutation(s) is known and in certain genetic isolates, mutation analysis may be performed. In addition, after a diagnosis is made by biochemical means, mutation analysis may be performed for certain disorders.

Treatment

There are no cures for lysosomal storage diseases and treatment is mostly symptomatic, although bone marrow transplantation and enzyme replacement therapy (ERT) have been tried with some success.^[2]^[3] In addition, umbilical cord blood transplantation is being performed at specialized centers for a number of these diseases. In addition, substrate reduction therapy, a method used to decrease the accumulation of storage material, is currently being evaluated for some of these diseases. Furthermore, chaperone therapy, a technique used to stabilize the defective enzymes produced by patients, is being examined for certain of these disorders. The experimental technique of gene therapy may offer cures in the future.^[4]

History

Tay-Sachs disease was the first of these disorders to be described, in 1881, followed by Gaucher disease in 1882. In the late 1950s and early 1960s, de Duve and colleagues, using cell fractionation techniques, cytological studies and biochemical analyses, identified and characterized the lysosome as a cellular organelle responsible for intracellular digestion and recycling of macromolecules. This was the scientific breakthrough that would lead to the understanding of the physiological basis of the Lysosomal Storage Diseases. Pompe disease was the first disease to be identified as an LSD in 1963, with L. Hers reporting the cause as a deficiency of α-glucosidase. Hers also suggested that other diseases, such as the Mucopolysaccharidosis, might be due to enzyme deficiencies.

Classification

Standard classification

The lysosomal storage diseases are generally classified by the nature of the primary stored material involved, and can be broadly broken into the following: (ICD-10 codes are provided where available)

(E75) lipid storage disorders, mainly sphingolipidoses (including Gaucher's and Niemann-Pick diseases)
- (E75.0-E75.1) gangliosidosis (including Tay-Sachs disease)
- (E75.2) leukodystrophies
(E76.0) mucopolysaccharidoses (including Hunter syndrome and Hurler disease)
(E77) glycoprotein storage disorders
(E77.0-E77.1) mucolipidoses

Also, Glycogen storage disease type II (Pompe disease) is also a defect in lysosomal metabolism,^[5] although it is otherwise classified into E74.0 in ICD-10.

By type of defect protein

Alternatively to the protein targets, lysosomal storage diseases may be classified by the type of protein that is deficient and is causing buildup.

Type of defect protein	Disease examples	Deficient protein
Lysosomal enzymes primarily	Tay-Sachs disease, I-cell disease^[6], Sphingolipidoses (e.g., gangliosidosis, Gaucher and Niemann-Pick disease)	Various
Posttranslational modification of enzymes	Multiple sulfatase deficiency	Multiple sulfatases
Membrane transport proteins	Mucolipidosis type II and IIIA	N-acetylglucosamine-1-phosphate transferase
Enzyme protecting proteins	Galactosialidosis	Cathepsin A
Soluble nonenzymatic proteins	GM2-AP deficiency, variant AB, Niemann-Pick disease, type C2	GM2-AP, NPC2
Transmembrane proteins	SAP deficiency	Sphingolipid activator proteins
	Niemann-Pick disease, type C1	NPC1
	Salla disease	Sialin
Unless else specified in boxes, then ref is:^[7]

Alphabetical list

Following are lysosomal storage diseases in alphabetical order:

Activator Deficiency/GM2 Gangliosidosis

Alpha-mannosidosis

Aspartylglucosaminuria

Cholesteryl ester storage disease

Chronic Hexosaminidase A Deficiency

Type I
Type II
Type III

GM1 gangliosidosis

Infantile
Late infantile/Juvenile
Adult/Chronic

I-Cell disease/Mucolipidosis II

Infantile Free Sialic Acid Storage Disease/ISSD

Juvenile Hexosaminidase A Deficiency

Krabbe disease

Infantile Onset
Late Onset

Lysosomal acid lipase deficiency

Early onset
Late onset

Metachromatic Leukodystrophy

Mucopolysaccharidoses disorders

Pseudo-Hurler polydystrophy/Mucolipidosis IIIA
MPSI Hurler Syndrome
MPSI Scheie Syndrome
MPS I Hurler-Scheie Syndrome
MPS II Hunter syndrome
Sanfilippo syndrome Type A/MPS III A
Sanfilippo syndrome Type B/MPS III B
Sanfilippo syndrome Type C/MPS III C
Sanfilippo syndrome Type D/MPS III D
Morquio Type A/MPS IVA
Morquio Type B/MPS IVB
MPS IX Hyaluronidase Deficiency
MPS VI Maroteaux-Lamy
MPS VII Sly Syndrome
Mucolipidosis I/Sialidosis
Mucolipidosis IIIC
Mucolipidosis type IV

Multiple sulfatase deficiency

Niemann-Pick Disease

Type A
Type B
Type C

Neuronal Ceroid Lipofuscinoses

CLN6 disease - Atypical Late Infantile, Late Onset variant, Early Juvenile
Batten-Spielmeyer-Vogt/Juvenile NCL/CLN3 disease
Finnish Variant Late Infantile CLN5
Jansky-Bielschowsky disease/Late infantile CLN2/TPP1 Disease
Kufs/Adult-onset NCL/CLN4 disease
Northern Epilepsy/variant late infantile CLN8
Santavuori-Haltia/Infantile CLN1/PPT disease
Beta-mannosidosis

Pompe disease/Glycogen storage disease type II

Pycnodysostosis

Sandhoff disease/Adult Onset/GM2 Gangliosidosis

Sandhoff disease/GM2 gangliosidosis - Infantile

Sandhoff disease/GM2 gangliosidosis - Juvenile

Schindler disease

Salla disease/Sialic Acid Storage Disease

Tay-Sachs/GM2 gangliosidosis

Wolman disease

References

^ Winchester B, Vellodi A, Young E (2000). "The molecular basis of lysosomal storage diseases and their treatment". Biochem. Soc. Trans. 28 (2): 150–4. PMID 10816117.
^ Clarke JT, Iwanochko RM (2005). "Enzyme replacement therapy of Fabry disease". Mol. Neurobiol. 32 (1): 043–050. doi:10.1385/MN:32:1:043. PMID 16077182.
^ Bruni S, Loschi L, Incerti C, Gabrielli O, Coppa GV (2007). "Update on treatment of lysosomal storage diseases". Acta Myol 26 (1): 87–92. PMC 2949325. PMID 17915580. http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pmcentrez&artid=2949325.
^ Ponder KP, Haskins ME (2007). "Gene therapy for mucopolysaccharidosis". Expert Opin Biol Ther 7 (9): 1333–1345. doi:10.1517/14712598.7.9.1333. PMID 17727324.
^ eMedicine Specialties > Neurology > Pediatric Neurology > Lysosomal Storage Disease Author: Noah S Scheinfeld, MD, JD, FAAD. Coauthor(s): Rowena Emilia Tabamo, MD; Brian Klein, MD. Updated: Sep 25, 2008
^ Medical Physiology (2nd Edition) – W. Boron & E. Boulpaep, Saunders Press
^ Table 7-6 in:Mitchell, Richard Sheppard; Kumar, Vinay; Abbas, Abul K.; Fausto, Nelson (2007). Robbins Basic Pathology. Philadelphia: Saunders. ISBN 1-4160-2973-7. 8th edition.

External links

(LSD) Inborn error of lipid metabolism: lipid storage disorders (E75, 272.7–272.8)

Sphingolipidoses
(to ceramide)

From ganglioside (gangliosidoses)	Ganglioside: GM1 gangliosidoses · GM2 gangliosidoses (Sandhoff disease, Tay-Sachs disease, AB variant)

From globoside	Globotriaosylceramide: Fabry's disease

From sphingomyelin	Sphingomyelin: phospholipid: Niemann–Pick disease (SMPD1-associated, type C) Glucocerebroside: Gaucher's disease

From sulfatide (sulfatidoses, leukodystrophy)	Sulfatide: Metachromatic leukodystrophy · Multiple sulfatase deficiency Galactocerebroside: Krabbe disease

To sphingosine	Ceramide: Farber disease

NCL

Infantile · Jansky-Bielschowsky disease · Batten disease

Other

Cerebrotendineous xanthomatosis · Cholesteryl ester storage disease (Lysosomal acid lipase deficiency/Wolman disease) · Sea-blue histiocyte syndrome

M: MET

mt, k, c/g/r/p/y/i, f/h/s/l/o/e, a/u, n, m

k, cgrp/y/i, f/h/s/l/o/e, au, n, m, epon

m(A16/C10),i(k, c/g/r/p/y/i, f/h/s/o/e, a/u, n, m)

(LSD) Inborn error of carbohydrate metabolism: mucopolysaccharidosis (E76, 277.5)

Anabolism

Pentosuria

Heparin sulfate: EXT1 (Hereditary multiple exostoses 1)

Chondroitin sulfate: PAPSS2 (Spondyloepimetaphyseal dysplasia, Pakistani type)

Catabolism

IDUA (1:Hurler/Scheie) · IDS (2:Hunter) · SGSH/NAGLU/HGSNAT/GNS (3:Sanfilippo ABCD) · GALNS/GLB1 (4:Morquio) · ARSB (6:Maroteaux-Lamy) · GUSB (7:Sly)

M: MET

mt, k, c/g/r/p/y/i, f/h/s/l/o/e, a/u, n, m

k, cgrp/y/i, f/h/s/l/o/e, au, n, m, epon

m(A16/C10),i(k, c/g/r/p/y/i, f/h/s/o/e, a/u, n, m)