myopathic facies

Mental Retardation, AD 31

Clinical Characteristics

Ocular Features:

A variety of ocular dysmorphisms have been described in this disorder including up-slanting lid fissures, epicanthal folds, hypertelorism, and telecanthus. Ptosis was described in 1 patient. Strabismus, nystagmus, and disconjugate gaze have been observed. Visual acuity has not been reported but "variable visual impairment" has been described. One patient was considered to have cortical visual impairment.

Systemic Features:

Neonatal hypotonia and feeding difficulties are among the first signs along with seizure-like activity (50%) including infantile spasms. EEG anomalies are present in the majority of individuals. Gastroscopy tubes may be required in a significant minority of patients. Hypotonic or myopathic facies is common. Apneic episodes may be seen in the neonatal period and most infants have respiratory difficulties in the first year of life which may improve during this period. Learning difficulties and features of autism are common. Some patients are unable to walk while others have an ataxic or broad-based gait. Speech may be absent or severely limited. The forehead is prominent while the hard palate is usually highly vaulted.

Brain MRIs may show delayed myelination but such scans have been described as normal in other individuals. Enlarged ventricles, a thin corpus callosum, and periventricular white matter changes may also be present. Neuropathologic studies have revealed chronic inflammatory changes around the arterioles of deep while matter.

Genetics

Heterozygous mutations in the PURA gene (5q31) have been identified in this disorder.

Pedigree:

Autosomal dominant

Treatment

Treatment Options:

No treatment has been reported.

References

Article Title:

Expanding the neurodevelopmental phenotype of PURA syndrome

Lee BH, Reijnders MRF, Abubakare O, Tuttle E, Lape B, Minks KQ, Stodgell C, Bennetto L, Kwon J, Fong CT, Gripp KW, Marsh ED, Smith WE, Huq AM, Coury SA, Tan WH, Solis O, Mehta RI, Leventer RJ, Baralle D, Hunt D, Paciorkowski AR. Expanding the neurodevelopmental phenotype of PURA syndrome. Am J Med Genet A. 2018 Jan;176(1):56-67.

PubMed ID:

29150892

De novo mutations in PURA are associated with hypotonia and developmental delay

Tanaka AJ, Bai R, Cho MT, Anyane-Yeboa K, Ahimaz P, Wilson AL, Kendall F, Hay B, Moss T, Nardini M, Bauer M, Retterer K, Juusola J, Chung WK. De novo mutations in PURA are associated with hypotonia and developmental delay. Cold Spring Harb Mol Case Stud. 2015 Oct;1(1):a000356. doi: 10.1101/mcs.a000356.

PubMed ID:

27148565

Mutations in PURA cause profound neonatal hypotonia, seizures, and encephalopathy in 5q31.3 microdeletion syndrome

Lalani SR, Zhang J, Schaaf CP, Brown CW, Magoulas P, Tsai AC, El-Gharbawy A, Wierenga KJ, Bartholomew D, Fong CT, Barbaro-Dieber T, Kukolich MK, Burrage LC, Austin E, Keller K, Pastore M, Fernandez F, Lotze T, Wilfong A, Purcarin G, Zhu W, Craigen WJ, McGuire M, Jain M, Cooney E, Azamian M, Bainbridge MN, Muzny DM, Boerwinkle E, Person RE, Niu Z, Eng CM, Lupski JR, Gibbs RA, Beaudet AL, Yang Y, Wang MC, Xia F. Mutations in PURA cause profound neonatal hypotonia, seizures, and encephalopathy in 5q31.3 microdeletion syndrome. Am J Hum Genet. 2014 Nov 6;95(5):579-83.

PubMed ID:

25439098

Whole exome sequencing in family trios reveals de novo mutations in PURA as a cause of severe neurodevelopmental delay and learning disability

Hunt D, Leventer RJ, Simons C, Taft R, Swoboda KJ, Gawne-Cain M; DDD study, Magee AC, Turnpenny PD, Baralle D. Whole exome sequencing in family trios reveals de novo mutations in PURA as a cause of severe neurodevelopmental delay and learning disability. J Med Genet. 2014 Dec;51(12):806-13.

PubMed ID:

25342064

Hypotonia, Infantile, with Psychomotor Retardation

Clinical Characteristics

Ocular Features:

Abducens nerve palsy with characteristic strabismus (esotropia) can be present.

Systemic Features:

Mothers may note decreased fetal movements. Severe generalized hypotonia can be evident at birth, requiring tube feeding and respiratory assistance. Death may occur before 6 months of age but with intense supportive care children can live for several years. Brain imaging may show enlarged lateral ventricles and thinning of the corpus callosum in some individuals but no abnormalities in others. Muscle biopsies can show severe myopathic changes with increased fibrosis, variation in fiber size, and small atrophic fibers. Cardiac septal defects have been reported. Delayed psychomotor development is a common feature.

Genetics

Homozygous mutations in the CCDC174 gene (3p25.1) are responsible for this condition so far reported in only two families with 6 children affected.

Pedigree:

Autosomal recessive

Treatment

Treatment Options:

No treatment is known for this condition.

References

Article Title:

CDC174, a novel

Volodarsky M, Lichtig H, Leibson T, Sadaka Y, Kadir R, Perez Y, Liani-Leibson
K, Gradstein L, Shaco-Levy R, Shorer Z, Frank D, Birk OS. CDC174, a novel
component of the exon junction complex whose mutation underlies a syndrome of
hypotonia and psychomotor developmental delay. Hum Mol Genet. 2015 Nov
15;24(22):6485-91.

PubMed ID:

26358778

Myotonic Dystrophy 1

Clinical Characteristics

Ocular Features:

Posterior subcapsular cataracts may be seen at any age, often with striking iridescent opacities in the overlying cortex as well. These polychromatic lens changes can be diagnostic but are present in only 50% of young adults with myotonic dystrophy. When present, they are almost always bilateral. Proximal muscle involvement leads to ptosis, strabismus, weakness of the orbicularis oculi, and sometimes ophthalmoplegia. Such muscle weakness may lead to exposure keratitis.

As many as 25% of patients with DM have a pigmentary retinopathy, usually in a butterfly pattern.

A low IOP and even hypotony is sometimes seen. The mean IOP in a series of 51 patients has been reported as 10.9 compared with 15.4 in controls. Using ultrasound biomicroscopy, ciliary body detachments were found in at least one quadrant of all eyes.

Systemic Features:

In the congenital form, hypotonia, generalized weakness, mental retardation and respiratory insufficiency are often present. There is a great deal of clinical heterogeneity among patients. Those with mild disease may have only cataracts and mild myotonia with a normal life expectancy. Those with more severe disease (classical myotonic dystrophy) have these signs plus marked muscle weakness and wasting. Cardiac conduction defects with secondary arryhthmias are a significant cause of mortality. Such patients tend to become disabled in adulthood. Symptoms become evident in the second decade or later. Deep muscle pain is common and can be severe. Distal muscle weakness usually begins before facial muscle weakness is apparent. Myotonia often involves the tongue while proximal muscle weakness can cause dysphagia and dysarthria. Such patients may also suffer respiratory distress. Reproductive fitness is reduced in males who can have gonadal atrophy. Frontal balding is common. Some age-related cognitive decline occurs.

Over 60% of patients have a hearing impairment and more than half of these have auditory brainstem response abnormalities. Vestibular hypesthesia is present in 37.5%.

Genetics

Myotonic dystrophy 1 is an autosomal dominant disorder caused by a trinucleotide (CTG) repeat expansion in a region of the DMPK gene (19q13.2-q13.3). The number of repeats varies widely and is roughly correlated with severity of disease. Infants with congenital myotonia usually have the highest number of repeats and have the most severe cognitive deficits. The number can expand during gametogenesis each generation (resulting in the phenomenon of anticipation) and females generally transmit larger numbers. Most infants with congenital myotonia are offspring of affected mothers. Reduced fetal movement and hydramnios are often noted during such pregnancies.

Affected males have few offspring secondary to gonadal atrophy. Affected heterozygous females, however, do not have the expected ratio of affected offspring because of the dynamic nature of the number of repeats. The risk of an affected offspring for a nulliparous afflicted female is only 3-9% and she has a 20-40% risk of recurrence after the birth of an affected child.

In a study of sibships with myotonic dystrophy, 58% of offspring were affected when the transmitting parent was male and 63% when the transmitting parent was female.

At least some of the variable transmission risks and clinical heterogeneity may be explained by somatic instability of the CTG repeat numbers. The degree of instability, moreover, may also be heritable. Age of onset, for example, is modified by the level of somatic instability. Further, patients in whom the repeat expands more rapidly develop symptoms earlier.

A similar disorder, myotonic dystrophy 2 (602668), is caused by a tetranucleotide repeat expansion in the CNBP gene.

Pedigree:

Autosomal dominant

Treatment

Treatment Options:

A variety of pharmaceutical agents have been tried for pain management without consistent results. No treatment improves the muscle weakness. Cholesterol lowering drugs such as statins should be avoided. Physical therapy may be helpful.

Cardiac conduction and structural defects are a significant threat even in asymtomatic patients and require constant monitoring for the development of arrythmias.

References

Article Title:

Myotonic Dystrophy Type 1 Management and Therapeutics

Smith CA, Gutmann L. Myotonic Dystrophy Type 1 Management and Therapeutics. Curr Treat Options Neurol. 2016 Dec;18(12):52. Review.

PubMed ID:

27826760

Structural and electrical cardiac abnormalities are prevalent in asymptomatic adults with myotonic dystrophy

Choudhary P, Nandakumar R, Greig H, Broadhurst P, Dean J, Puranik R, Celermajer DS, Hillis GS. Structural and electrical cardiac abnormalities are prevalent in asymptomatic adults with myotonic dystrophy. Heart. 2016 May 10. pii: heartjnl-2015-308517. doi: 10.1136/heartjnl-2015-308517. [Epub ahead of print] PubMed PMID: 27164920.

PubMed ID:

27164920

Inner ear dysfunction in myotonic dystrophy type 1

Balatsouras DG, Felekis D, Panas M, Xenellis J, Koutsis G, Kladi A, Korres SG. Inner ear dysfunction in myotonic dystrophy type 1. Acta Neurol Scand. 2012 Nov 5. doi: 10.1111/ane.12020. [Epub ahead of print].

PubMed ID:

23121018

The heart and cardiac pacing in Steinert disease

Nigro G, Papa AA, Politano L. The heart and cardiac pacing in Steinert disease. Acta Myol. 2012 Oct;31(2):110-6.

PubMed ID:

23097601

Butterfly-shaped Pattern Dystrophy in Myotonic Dystrophy

Makino S, Ohkubo Y, Tampo H. Butterfly-shaped Pattern Dystrophy in Myotonic Dystrophy. Intern Med. 2012;51(16):2253-4. Epub 2012 Aug 15.

PubMed ID:

22892517

Somatic instability of the expanded CTG triplet repeat in myotonic dystrophy type 1 is a heritable quantitative trait and modifier of disease severity

les F, Couto JM, Higham CF, Hogg G, Cuenca P, Braida C, Wilson RH, Adam B, Del Valle G, Brian R, Sittenfeld M, Ashizawa T, Wilcox A, Wilcox DE, Monckton DG. Somatic instability of the expanded CTG triplet repeat in myotonic dystrophy type 1 is a heritable quantitative trait and modifier of disease severity. Hum Mol Genet. 2012 May 16. [Epub ahead of print].

PubMed ID:

22595968

Low intraocular pressure resulting from ciliary body detachment in patients with myotonic dystrophy

Rosa N, Lanza M, Borrelli M, De Bernardo M, Palladino A, Di Gregorio MG, Pascotto F, Politano L. Low intraocular pressure resulting from ciliary body detachment in patients with myotonic dystrophy. Ophthalmology. 2011 Feb;118(2):260-4.

PubMed ID:

20801513

Segregation distortion in myotonic dystrophy

Magee AC, Hughes AE. Segregation distortion in myotonic dystrophy. J Med Genet. 1998 Dec;35(12):1045-6.

PubMed ID:

9863607

Retinal changes in myotonic dystrophy. Clinical and follow-up evaluation

Kimizuka Y, Kiyosawa M, Tamai M, Takase S. Retinal changes in myotonic dystrophy. Clinical and follow-up evaluation. Retina. 1993;13(2):129-35.

PubMed ID:

8337494

Diagnostic value of ophthalmologic findings in myotonic dystrophy: comparison with risks calculated by haplotype analysis of closely linked restriction fragment length polymorphisms

Ashizawa T, Hejtmancik JF, Liu J, Perryman MB, Epstein HF, Koch DD. Diagnostic value of ophthalmologic findings in myotonic dystrophy: comparison with risks calculated by haplotype analysis of closely linked restriction fragment length polymorphisms. Am J Med Genet. 1992 Jan 1;42(1):55-60.

PubMed ID:

1364051

Incidence and predictors of sudden death, major conduction defects and sustained ventricular tachyarrhythmias in 1388 patients with myotonic dystrophy type 1

Wahbi K, Babuty D, Probst V, Wissocque L, Labombarda F, Porcher R, Becane HM, Lazarus A, Behin A, Laforet P, Stojkovic T, Clementy N, Dussauge AP, Gourraud JB, Pereon Y, Lacour A, Chapon F, Milliez P, Klug D, Eymard B, Duboc D. Incidence and predictors of sudden death, major conduction defects and sustained ventricular tachyarrhythmias in 1388 patients with myotonic dystrophy type 1. Eur Heart J. 2016 Dec 9. pii: ehw569. [Epub ahead of print] PubMed.

PubMed ID:

27941019

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