Morquio syndrome: Difference between revisions

Morquio syndrome
Synonyms	Mucopolysaccharidosis type IV (MPS IV)
Pronounce
Specialty	Medical genetics
Symptoms	Short stature, skeletal abnormalities, joint laxity, corneal clouding
Complications	N/A
Onset	Early childhood
Duration	Lifelong
Types	N/A
Causes	Genetic mutation in GALNS or GLB1 genes
Risks	Family history
Diagnosis	Clinical evaluation, genetic testing
Differential diagnosis	Achondroplasia, Spondyloepiphyseal dysplasia
Prevention	N/A
Treatment	Enzyme replacement therapy, supportive care
Medication	Elosulfase alfa
Prognosis	Variable, depends on severity
Frequency	1 in 200,000 to 300,000 live births
Deaths

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Morquio syndrome, clinically recognized as Mucopolysaccharidosis Type IV (MPS IV), is a rare and inherited metabolic disorder. Patients with this syndrome lack the necessary enzymes to break down a specific group of sugar molecules termed glycosaminoglycans (often abbreviated as GAGs or mucopolysaccharides). The accumulation of these GAGs, primarily keratan sulfate, leads to multi-organ dysfunction and various associated symptoms.

Genetic Foundation[edit]

Morquio syndrome is an autosomal recessive birth defect, implying that a child must inherit two copies of the defective gene (one from each parent) to manifest the disorder. The underlying defect is categorized under lysosomal storage disorders, wherein the body's lysosomes fail to degrade waste molecules, resulting in their accumulation.

Glycosaminoglycans and Their Role[edit]

Glycosaminoglycans (GAGs) play a pivotal role in the matrix of many tissues. Under normal circumstances, they undergo constant turnover - synthesis followed by degradation. In Morquio syndrome, the degradation pathway is interrupted due to enzyme deficiencies.

Keratan sulfate: Particularly important in Morquio syndrome, it's predominantly found in the cornea, cartilage, and bone. The inability to degrade keratan sulfate leads to its systemic buildup.

Symptoms and Organ Systems Affected[edit]

Morquio syndrome's clinical presentation varies, resulting from the deposition of GAGs in different body parts:

Skeletal system: Most individuals exhibit skeletal abnormalities, such as short stature, knock-knees, and abnormalities in the neck vertebrae.
Respiratory system: Airway obstruction and pulmonary complications are commonly observed.
Cardiovascular system: Heart valve disease and coronary artery complications can arise.
Vision: Corneal clouding leading to visual impairment.
Hearing: Progressive hearing loss can occur due to recurrent ear infections and buildup of GAGs.
Mobility: Joint issues can restrict movement and cause pain.

Signs and symptoms[edit]

Patients with Morquio syndrome appear healthy at birth. Types A and B have similar presentations, but Type B generally has milder symptoms. The age of onset is usually between 1 and 3 years of age. Morquio syndrome causes progressive changes to the skeleton of the ribs and chest, which may lead to neurological complications such as nerve compression. Patients may also have hearing loss and clouded corneas. Intelligence is usually normal unless a patient suffers from untreated hydrocephalus. Physical growth slows and often stops around age 8. Skeletal abnormalities include a bell-shaped chest, a flattening or curvature of the spine, shortened long bones, and dysplasia of the hips, knees, ankles, and wrists. The bones that stabilize the connection between the head and neck can be malformed (odontoid hypoplasia); in these cases, a surgical procedure called spinal cervical bone fusion can be lifesaving. Restricted breathing, joint stiffness, and heart disease are also common. Children with the more severe form of MPS IV may not live beyond their twenties or thirties.

Cause[edit]

Morquio syndrome is inherited from an autosomal recessive inherited gene. Every person has two copies of the genes needed to break down keratan sulfate, but only one healthy copy is needed. Both parents pass down one defective copy to their child, resulting in a child with no functional copies of the gene. As such, the body is incapable breaking down keratan sulfate for disposal. The incompletely broken down GAGs remain stored in cells in the body, causing progressive damage. Babies may show little sign of the disease, but as more and more cells become damaged, symptoms start to appear.

Diagnosis[edit]

Classification[edit]

This syndrome has two forms, A and B, referred to as Morquio A and Morquio B syndrome or MPS IVA and MPS IVB. The two forms are distinguished by the gene product involved; Type A involves a malfunction in the GALNS gene, while Type B involves a malfunction of the GLB1 gene.

Genetics of MPS IV
Morquio syndrome type	Gene	Missing enzyme	Chromosomal region
Type A	GALNS	Galactosamine-6 sulfatase	16q24
Type B	GLB1	Beta-galactosidase	3p22

Treatment[edit]

The treatment for Morquio syndrome consists of prenatal identification and of enzyme replacement therapy. On 12 February 2014, the US Food and Drug Administration approved the drug elosulfase alfa (Vimizim) for treating Type A. Currently, there is no treatment for Type B.

Prognosis[edit]

The lifespan of patients with Morquio syndrome is variable and depends on the subtype. Type A is generally severe, with a life expectancy in the 20s to 30s.

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@@ Line 1: / Line 1: @@
-== Morquio Syndrome: An Overview ==
+{{SI}}
+{{Infobox medical condition
-[[File:Mucopolysaccharidosis (Morquio's Disease) 3.jpg|thumb|right|300px|Morquio syndrome's impact on the human skeletal structure.]]
+| name            = Morquio syndrome
+| image           = [[File:Mucopolysaccharidosis_(Morquio's_Disease)_1.jpg|alt=Morquio syndrome]]
+| caption         = X-ray of a patient with Morquio syndrome
+| synonyms        = Mucopolysaccharidosis type IV (MPS IV)
+| pronounce       =
+| specialty       = [[Medical genetics]]
+| symptoms        = Short stature, skeletal abnormalities, joint laxity, corneal clouding
+| onset           = Early childhood
+| duration        = Lifelong
+| causes          = Genetic mutation in [[GALNS]] or [[GLB1]] genes
+| risks           = Family history
+| diagnosis       = Clinical evaluation, genetic testing
+| differential    = [[Achondroplasia]], [[Spondyloepiphyseal dysplasia]]
+| treatment       = [[Enzyme replacement therapy]], supportive care
+| medication      = [[Elosulfase alfa]]
+| prognosis       = Variable, depends on severity
+| frequency       = 1 in 200,000 to 300,000 live births
+| deaths          =
+}}
+[[File:Mucopolysaccharidosis (Morquio's Disease) 3.jpg|left|thumb|300px|Morquio syndrome's impact on the human skeletal structure.]]
 '''Morquio syndrome''', clinically recognized as '''[[Mucopolysaccharidosis]] Type IV (MPS IV)''', is a rare and inherited [[metabolic disorder]]. Patients with this syndrome lack the necessary enzymes to break down a specific group of sugar molecules termed [[glycosaminoglycans]] (often abbreviated as GAGs or mucopolysaccharides). The accumulation of these GAGs, primarily [[keratan sulfate]], leads to multi-organ dysfunction and various associated symptoms.
 == Genetic Foundation ==
 Morquio syndrome is an [[autosomal recessive]] [[birth defect]], implying that a child must inherit two copies of the defective gene (one from each parent) to manifest the disorder. The underlying defect is categorized under [[lysosomal storage disorders]], wherein the body's lysosomes fail to degrade waste molecules, resulting in their accumulation.
 == Glycosaminoglycans and Their Role ==
 [[Glycosaminoglycans]] (GAGs) play a pivotal role in the matrix of many tissues. Under normal circumstances, they undergo constant turnover - synthesis followed by degradation. In Morquio syndrome, the degradation pathway is interrupted due to enzyme deficiencies.
 * '''[[Keratan sulfate]]''': Particularly important in Morquio syndrome, it's predominantly found in the cornea, cartilage, and bone. The inability to degrade keratan sulfate leads to its systemic buildup.
 == Symptoms and Organ Systems Affected ==
 Morquio syndrome's clinical presentation varies, resulting from the deposition of GAGs in different body parts:
 * '''Skeletal system''': Most individuals exhibit skeletal abnormalities, such as short stature, knock-knees, and abnormalities in the neck vertebrae.
 * '''Respiratory system''': Airway obstruction and pulmonary complications are commonly observed.
@@ Line 26: / Line 35: @@
 * '''Hearing''': Progressive hearing loss can occur due to recurrent ear infections and buildup of GAGs.
 * '''Mobility''': Joint issues can restrict movement and cause pain.
 == Signs and symptoms ==
+[[File:Corneal Clouding in MPS-VI (Maroteaux-Lamy Syndrome).jpg|left|thumb|Corneal clouding in a 30-year-old male with MPS VI. Morquio syndrome and other MPS disorders may also present with corneal clouding]]
-[[File:Corneal Clouding in MPS-VI (Maroteaux-Lamy Syndrome).jpg|thumb|right|Corneal clouding in a 30-year-old male with MPS VI. Morquio syndrome and other MPS disorders may also present with corneal clouding]]
 Patients with Morquio syndrome appear healthy at birth. Types A and B have similar presentations, but Type B generally has milder symptoms. The age of onset is usually between 1 and 3 years of age. Morquio syndrome causes progressive changes to the skeleton of the ribs and chest, which may lead to neurological complications such as nerve compression. Patients may also have hearing loss and clouded corneas. Intelligence is usually normal unless a patient suffers from untreated [[hydrocephalus]].
 Physical growth slows and often stops around age 8. Skeletal abnormalities include a bell-shaped chest, a flattening or curvature of the spine, shortened long bones, and dysplasia of the hips, knees, ankles, and wrists. The bones that stabilize the connection between the head and neck can be malformed (odontoid hypoplasia); in these cases, a surgical procedure called [[Spinal fusion|spinal cervical bone fusion]] can be lifesaving. Restricted breathing, joint stiffness, and heart disease are also common. Children with the more severe form of MPS IV may not live beyond their twenties or thirties.
 ==Cause==
-Morquio syndrome is inherited from an [[autosomal recessive]] inherited gene. Every person has two copies of the genes needed to break down keratan sulfate, but only one healthy copy is needed. Both parents pass down one defective copy to their child, resulting in a child with no functional copies of the gene. As such, the body is incapable breaking down keratan sulfate for disposal. The incompletely broken down GAGs remain stored in cells in the body, causing progressive damage. Babies may show little sign of the disease, but as more and more cells become damaged, symptoms start to appear.<ref name=CanadianMPS>{{cite web|url=https://www.mpssociety.ca/education/what-is-mps/what-is-mps-iv/ |title=MPS IV (Morquio Syndrome)|publisher=[[Canadian MPS Society]] |accessdate=14 June 2019}}</ref>
+Morquio syndrome is inherited from an [[autosomal recessive]] inherited gene. Every person has two copies of the genes needed to break down keratan sulfate, but only one healthy copy is needed. Both parents pass down one defective copy to their child, resulting in a child with no functional copies of the gene. As such, the body is incapable breaking down keratan sulfate for disposal. The incompletely broken down GAGs remain stored in cells in the body, causing progressive damage. Babies may show little sign of the disease, but as more and more cells become damaged, symptoms start to appear.
 ==Diagnosis==
 === Classification ===
 This syndrome has two forms, A and B, referred to as Morquio A and Morquio B syndrome or MPS IVA and MPS IVB. The two forms are distinguished by the gene product involved; Type A involves a malfunction in the [[GALNS]] gene, while Type B involves a malfunction of the [[GLB1]] gene.
 {| class="wikitable"
 |+ Genetics of MPS IV
@@ Line 51: / Line 54: @@
 | [[GLB1]] || [[Beta-galactosidase]] || 3p22
 |}
 ==Treatment==
-The treatment for Morquio syndrome consists of [[prenatal diagnosis|prenatal identification]] and of [[enzyme replacement therapy]]. On 12 February 2014, the [[US Food and Drug Administration]] approved the drug [[elosulfase alfa]] (Vimizim) for treating Type A. Currently, there is no treatment for Type B.<ref name=CanadianMPS />
+The treatment for Morquio syndrome consists of [[prenatal diagnosis|prenatal identification]] and of [[enzyme replacement therapy]]. On 12 February 2014, the [[US Food and Drug Administration]] approved the drug [[elosulfase alfa]] (Vimizim) for treating Type A. Currently, there is no treatment for Type B.
 ==Prognosis==
-The lifespan of patients with Morquio syndrome is variable and depends on the subtype. Type A is generally severe, with a life expectancy in the 20s to 30s. <ref name=NINDS>{{cite web|title=Mucopolysaccharidoses Fact Sheet| url=https://www.ninds.nih.gov/Disorders/Patient-Caregiver-Education/Fact-Sheets/Mucopolysaccharidoses-Fact-Sheet| date=13 May 2019 |accessdate=14 June 2019 |publisher=[[National Institute of Neurological Disorders and Stroke]]}}</ref> In 2016, a man with Morquio syndrome died at the age of 81.<ref>{{cite web|url=http://och-c.com/?q=content/kenneth-dean-martin |title=Kenneth Dean Martin |publisher=[[Osage County Herald-Chronicle]] |date=23 September 2016 |accessdate=14 June 2019 |last=Blacketer |first=Rosie}}</ref>
+The lifespan of patients with Morquio syndrome is variable and depends on the subtype. Type A is generally severe, with a life expectancy in the 20s to 30s.
-One study found that the mean life expectancy for patients in the [[United Kingdom]] was 25.30, with a [[standard deviation]] of 17.43 years. On average, female patients lived 4 years longer than male patients. [[Respiratory failure]] was the primary cause of death in 63% of patients. Other causes of death were cardiac failure (11%), post-traumatic organ failure (11%), complications of surgery (11%), and [[heart attack]] (4%). Life expectancy has been increasing since the 1980s. The average age at death due to respiratory failure improved from 17.42 years old in the 1980s to 30.74 years old in the 2000s.<ref name=Lavery>{{cite journal|title=Mortality in Patients with Morquio Syndrome A |last1=Lavery |first1=Christine |last2=Hendriksz |first2=Chris |date=10 Apr 2014 |pmid=24718838 |journal=[[Journal of Inherited Metabolic Disease]] |pmc=4270860 |doi=10.1007/8904_2014_298 |volume=15 |pages=59–66|series=JIMD Reports }}</ref>
-== History ==
-The condition was first described, simultaneously and independently, in 1929, by [[Luis Morquio]] (1867–1935),<ref>{{cite journal |first=L.|last=Morquio |title=Sur une forme de dystrophie osseuse familiale |journal=Archives de Médecine des Infants |location=Paris |year=1929 |volume=32 |issue= |pages=129–135 |doi= |pmid= |issn=0365-4311 }}</ref> a prominent [[Uruguay]]an physician who discovered it in [[Montevideo]], and [[James Frederick Brailsford]] (1888–1961), an English radiologist in [[Birmingham]], [[England]].<ref>{{WhoNamedIt|synd|2108}}</ref><ref>{{cite journal |first=J. F. |last=Brailsford |title=Chondro-osteo-dystrophy: Roentgenographic & clinical features of a child with dislocation of vertebrae |journal=American Journal of Surgery |location= New York |year=1929 |volume=7 |issue=3 |pages=404–410 |doi=10.1016/S0002-9610(29)90496-7 |pmid= }}</ref> They both recognized the occurrence of [[cornea]]l clouding, [[aorta|aortic]] valve disease, and urinary excretion of keratan sulfate. Morquio observed the disorder in four siblings in a family of Swedish descent and reported his observations in French.
-== See also ==
-* [[Hurler syndrome]] ([[Mucopolysaccharidosis type I|MPS I]])
-* [[Hunter syndrome]] (MPS II)
-* [[Sanfilippo syndrome]] (MPS III)
-* [[Dwarfism]]
-== References ==
-{{reflist}}
-== External links ==
-{{Medical resources
-|   DiseasesDB     = 30807
-|    ICD10          = {{ICD10|E|76|2|e|70}}
-|   ICD9           = {{ICD9|277.5}}
-|   ICDO           =
-|   OMIM           = 253000
-|   OMIM_mult      = {{OMIM|253010||none}}
-|    MedlinePlus    = 001206
-|   eMedicineSubj  = ped
-|   eMedicineTopic = 1477
-|   MeshID         = D009085
-|   Orphanet       = 582
-}}
-{{Mucopolysaccharidoses}}
-== Diagnosis and Treatment ==
-Diagnosis typically involves:
-* '''Clinical examination''': Identification of physical abnormalities and symptoms.
-* '''Urine tests''': Increased GAG levels can be detected in the urine.
-* '''Genetic testing''': To confirm the presence of the defective gene.
-For treatment:
-* '''Enzyme replacement therapy (ERT)''': Introduction of the missing enzyme can help reduce the accumulation of GAGs.
-* '''Bone marrow transplant''': Though risky, it has been employed in some cases to introduce cells that produce the missing enzyme.
-* '''Supportive care''': Physiotherapy, surgery for skeletal issues, and management of respiratory and cardiac complications.
-== Conclusion ==
-Morquio syndrome, a type of [[Mucopolysaccharidosis]], emphasizes the importance of intricate metabolic pathways in human health. While treatment options are continually advancing, early diagnosis and multidisciplinary care remain vital for improving the quality of life of affected individuals.
 [[Category:Health]]
 [[Category:Medical Conditions]]

Morquio syndrome

Synonyms	Mucopolysaccharidosis type IV (MPS IV)
Pronounce
Specialty	Medical genetics
Symptoms	Short stature, skeletal abnormalities, joint laxity, corneal clouding
Complications	N/A
Onset	Early childhood
Duration	Lifelong
Types	N/A
Causes	Genetic mutation in GALNS or GLB1 genes
Risks	Family history
Diagnosis	Clinical evaluation, genetic testing
Differential diagnosis	Achondroplasia, Spondyloepiphyseal dysplasia
Prevention	N/A
Treatment	Enzyme replacement therapy, supportive care
Medication	Elosulfase alfa
Prognosis	Variable, depends on severity
Frequency	1 in 200,000 to 300,000 live births
Deaths