Becker's muscular dystrophy: Difference between revisions

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== Historical Perspective ==
== Historical Perspective ==
Becker's muscular [[dystrophy]] was first described by Peter Emil Becker, a German [[neurologist]], [[psychiatrist]] and [[geneticist]], in 1953 with his thesis called ‘‘Dystrophia Musculorum Progessiva: A [[Genetic]] and Clinical Investigation of the Muscular Dystrophies’’, after his work was interrumpted in 1942 due to [[World war|WWII]] recruitment. 


Before Becker, in the 1860's, French [[neurologist]] [[Guillaume Benjamin Amand Duchenne]] described in detail a slowly progessive [[Muscle weakness|muscular weakness]] in a boy, later known as [[Duchenne muscular dystrophy]].
* Becker's muscular [[dystrophy]] was first described by Peter Emil Becker, a German [[neurologist]], [[psychiatrist]] and [[geneticist]], in 1953 with his thesis called ‘‘Dystrophia Musculorum Progessiva: A [[Genetic]] and Clinical Investigation of the Muscular Dystrophies’’, after his work was interrumpted in 1942 due to [[World war|WWII]] recruitment. 
 
* Before Becker, in the 1860's, French [[neurologist]] [[Guillaume Benjamin Amand Duchenne]] described in detail a slowly progessive [[Muscle weakness|muscular weakness]] in a boy, later known as [[Duchenne muscular dystrophy]].
The association between [[genetic mutations]] and Duchenne [[muscular dystrophy]] was made in 1986.
* The association between [[genetic mutations]] and Duchenne [[muscular dystrophy]] was made in 1986.
 
* In 1987, [[dystrophin]] gene on [[X chromosome]] were first implicated in the [[pathogenesis]] of Becker's [[muscular dystrophy]]. <br />
In 1987, [[dystrophin]] gene on [[X chromosome]] were first implicated in the [[pathogenesis]] of Becker's [[muscular dystrophy]].
<br />


== Pathophysiology ==
== Pathophysiology ==
The [[pathogenesis]] of Becker's muscular [[dystrophy]] is characterized by muscle [[Muscle weakness|weakness]] and [[pseudohypertrophy]] (mostly [[proximal]]), [[Hypertrophic cardiomyopathy|cardiomyopathy]], elevated [[CK]] and skelletal [[Deformity|deformities]].
Becker's muscular dystrophy is inherited in an [[X-linked]] recessive fashion.
Becker's muscular [[dystrophy]] is caused by a [[mutation]] in the gene [[DMD]], one of the largest [[genes]] in humans. This [[gene]] encodes for the [[3685Y]] [[aminoacid]] protein called [[dystrophin]], wich can be found in [[Skeletal muscle|skeletal]] and [[Cardiac muscle cell|cardiac muscle]], among other tisues.  This [[mutation]] produces a truncated [[dystrophin]] [[protein]] that will translate into a decreased but not incomplete functionality (difference from [[Duchenne muscular dystrophy|Duchenne]]). Around 33% of patients with Becker's muscular dystrophy have [[de novo]] [[Mutation|mutations]]. Point [[Mutation|mutations]] and [[duplications]] appear mostly from [[spermatogenesis]] while deletions arise from [[oogenesis]] in most of te cases. 


On microscopic [[Histopathology|histopathological]] analysis, endomysial fibrosis with fatty replacement of [[muscle]] in later stages, [[inflammation]], increased internal [[nuclei]], [[Myofiber|myofibe]]<nowiki/>r cleavage with [[necrosis]], and [[phagocytosis]] are characteristic findings of Becker's muscular dystrophy.<ref name=":0" />
* The [[pathogenesis]] of Becker's muscular [[dystrophy]] is characterized by muscle [[Muscle weakness|weakness]] and [[pseudohypertrophy]] (mostly [[proximal]]), [[Hypertrophic cardiomyopathy|cardiomyopathy]], elevated [[CK]] and skelletal [[Deformity|deformities]].
<br />
* Becker's muscular dystrophy is inherited in an [[X-linked]] recessive fashion.
* Becker's muscular [[dystrophy]] is caused by a [[mutation]] in the gene [[DMD]], one of the largest [[genes]] in humans. This [[gene]] encodes for the [[3685Y]] [[aminoacid]] protein called [[dystrophin]], wich can be found in [[Skeletal muscle|skeletal]] and [[Cardiac muscle cell|cardiac muscle]], among other tisues.  This [[mutation]] produces a truncated [[dystrophin]] [[protein]] that will translate into a decreased but not incomplete functionality (difference from [[Duchenne muscular dystrophy|Duchenne]]). Around 33% of patients with Becker's muscular dystrophy have [[de novo]] [[Mutation|mutations]]. Point [[Mutation|mutations]] and [[duplications]] appear mostly from [[spermatogenesis]] while deletions arise from [[oogenesis]] in most of te cases. 
* On microscopic [[Histopathology|histopathological]] analysis, endomysial fibrosis with fatty replacement of [[muscle]] in later stages, [[inflammation]], increased internal [[nuclei]], [[Myofiber|myofibe]]<nowiki/>r cleavage with [[necrosis]], and [[phagocytosis]] are characteristic findings of Becker's muscular dystrophy.<ref name=":0" /> <br />


== Clinical Features ==
== Clinical Features ==
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== Screening ==
== Screening ==
[[Prenatal testing|Prenatal molecular genetic testing]] is recomended in couples planning to [[Pregnancy|conceive]] and have family members who are afected by or are [[Genetic carrier|carriers]] of a dystrophinopathy.
[[In utero|In-utero]] fetal [[muscle biopsy]] has also been realized under couples request for [[fetuses]] with a high [[probability]] of beign affected and inconclusive [[genetic linkage]].


It is important to identify females at risk to be [[heterozygous]] of a [[dystrophinopathy]], in order to manage possible [[Cardiomyopathies|cardiac]] complications; this can be done by [[Genetic testing|molecular genetic testing]], [[CK]] measurements, and [[Genetic linkage|linkage]] analysis.
* [[Prenatal testing|Prenatal molecular genetic testing]] is recomended in couples planning to [[Pregnancy|conceive]] and have family members who are afected by or are [[Genetic carrier|carriers]] of a dystrophinopathy.
* [[In utero|In-utero]] fetal [[muscle biopsy]] has also been realized under couples request for [[fetuses]] with a high [[probability]] of beign affected and inconclusive [[genetic linkage]].
* It is important to identify females at risk to be [[heterozygous]] of a [[dystrophinopathy]], in order to manage possible [[Cardiomyopathies|cardiac]] complications; this can be done by [[Genetic testing|molecular genetic testing]], [[CK]] measurements, and [[Genetic linkage|linkage]] analysis.


<br />
<br />


== Epidemiology and Demographics ==
== Epidemiology and Demographics ==
The [[prevalence]] of Becker's muscular dystrophy is approximately 1-3 per 100,000 individuals.


The [[incidence]] of Becker's muscular dystrophy is approximately 3-6 per 100,000 male [[births]] worldwide.<ref name=":1" /><ref name=":2" />  
* The [[prevalence]] of Becker's muscular dystrophy is approximately 1-3 per 100,000 individuals.
* The [[incidence]] of Becker's muscular dystrophy is approximately 3-6 per 100,000 male [[births]] worldwide.<ref name=":1" /><ref name=":2" />  


=== Age ===
=== Age ===
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=== Race ===
=== Race ===
Becker's muscular dystrophy usually affects individuals of the hispanic race.<ref name="pmid19834452" />


Asian individuals are less likely to develop Becker's muscular dystrophy.<ref name=":3" />
* Becker's muscular dystrophy usually affects individuals of the hispanic race.<ref name="pmid19834452" />
* Asian individuals are less likely to develop Becker's muscular dystrophy.<ref name=":3" />


== Risk Factors ==
== Risk Factors ==
Becker's muscular dystrophy is developed in the majority of cases from males who are born from [[genetic carrier]] mothers or by [[Mutation|spontaneous mutation]],<ref name="pmid23620649" /> there has not been any [[Risk factor|risk factors]] implicated for a [[DMD]] gene mutation.


Studies have found that several [[Genetics|genetic]] [[polymorphisms]] and [[Mutation|mutations]] may be a factor for Becker's muscular dystrophy progression, but further [[research]] is necessary to draw conclusions.
* Becker's muscular dystrophy is developed in the majority of cases from males who are born from [[genetic carrier]] mothers or by [[Mutation|spontaneous mutation]],<ref name="pmid23620649" /> there has not been any [[Risk factor|risk factors]] implicated for a [[DMD]] gene mutation.
<br />
* Studies have found that several [[Genetics|genetic]] [[polymorphisms]] and [[Mutation|mutations]] may be a factor for Becker's muscular dystrophy progression, but further [[research]] is necessary to draw conclusions. <br />
== Natural History, Complications and Prognosis ==
== Natural History, Complications and Prognosis ==
The majority of patients with Becker's muscular [[dystrophy]] remain [[asymptomatic]] until [[adolescence]].
Early clinical features include calf hypertrophy, difficulty rising from a chair, [[Anatomical terms of location|proximal]] muscle [[Muscle weakness|weakness]], climbing stairs, sustaining [[Imbalance|balance]], elevating arms, and in later stages [[heart failure]].<ref name="pmid20301298" />
The most common complications in Becker's muscular dystrophy are [[Cardiac failure|cardiac]] and [[Respiratory failure|respiratory]] failure, [[Pneumonia|pneumonias]], and in rare cases [[cognitive impairment]].
[[Prognosis]] is generally poor, depending on [[spectrum]] of Becker's muscular dystrophy, but much better that [[Duchenne muscular dystrophy]]. In 2002, the [[Survival analysis|survival]] rate at age 20 was 60%.
If left [[untreated]], the majority of patients with Becker's muscular dystrophy may die due to [[Cardiac failure|cardiac]] and [[Respiratory failure|respiratory]] failure in their mid-40's.


Cradiac, respiratory, and orthopedic care has greatly improved in last years for patients with Becker disease, this, increasing the life span in these individuals.<ref name=":4" />
* The majority of patients with Becker's muscular [[dystrophy]] remain [[asymptomatic]] until [[adolescence]].
* Early clinical features include calf hypertrophy, difficulty rising from a chair, [[Anatomical terms of location|proximal]] muscle [[Muscle weakness|weakness]], climbing stairs, sustaining [[Imbalance|balance]], elevating arms, and in later stages [[heart failure]].<ref name="pmid20301298" />
* The most common complications in Becker's muscular dystrophy are [[Cardiac failure|cardiac]] and [[Respiratory failure|respiratory]] failure, [[Pneumonia|pneumonias]], and in rare cases [[cognitive impairment]].
* [[Prognosis]] is generally poor, depending on [[spectrum]] of Becker's muscular dystrophy, but much better that [[Duchenne muscular dystrophy]]. In 2002, the [[Survival analysis|survival]] rate at age 20 was 60%.
* If left [[untreated]], the majority of patients with Becker's muscular dystrophy may die due to [[Cardiac failure|cardiac]] and [[Respiratory failure|respiratory]] failure in their mid-40's.
* Cradiac, respiratory, and orthopedic care has greatly improved in last years for patients with Becker disease, this, increasing the life span in these individuals.<ref name=":4" />


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<br />
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=== Medical Therapy ===
=== Medical Therapy ===
There is no definitive treatment for Becker's muscular [[dystrophy]]; treatment will be [[Multidisciplinary care|multidisciplinary]] depending on [[Comorbidity|comorbidities]]; the mainstay of therapy is [[supportive care]].


[[Corticosteroid medications|Corticosteroids]] have shown to improve strength in other [[dystrophinopathies]], but its efficacy on Beckers muscular dystrophy is uncertain. To measure improvement with [[corticosteroid]] therapy, [[timed muscle function tests]], [[pulmonary function tests]], and age at loss of [[independent ambulation]] are registered.<ref name="pmid2030129812" />
* There is no definitive treatment for Becker's muscular [[dystrophy]]; treatment will be [[Multidisciplinary care|multidisciplinary]] depending on [[Comorbidity|comorbidities]]; the mainstay of therapy is [[supportive care]].
* [[Corticosteroid medications|Corticosteroids]] have shown to improve strength in other [[dystrophinopathies]], but its efficacy on Beckers muscular dystrophy is uncertain. To measure improvement with [[corticosteroid]] therapy, [[timed muscle function tests]], [[pulmonary function tests]], and age at loss of [[independent ambulation]] are registered.<ref name="pmid2030129812" />
* The management of [[Scoliosis (patient information)|scoliosis]] is bracing and [[surgery]] in some cases.
* [[Beta-blockers]], [[ARBs|angiotensin II-receptor blockers]], and [[ACE inhibitor|ACE inhibitors]] are used to improve [[ventricular function]] in patients with Becker's muscular [[dystrophy]] when [[Ejection fraction|EF]] is less than 55%.
* [[Physical exercise|Low impact exercise]] (eg. [[swimming]]) should be advised. If [[myalgia]] presents, [[Physical exercise|physical activity]] should be reduced and [[myoglobinuria]] cheked out.


The management of [[Scoliosis (patient information)|scoliosis]] is bracing and [[surgery]] in some cases.
=== Surgery ===
 
[[Beta-blockers]], [[ARBs|angiotensin II-receptor blockers]], and [[ACE inhibitor|ACE inhibitors]] are used to improve [[ventricular function]] in patients with Becker's muscular [[dystrophy]] when [[Ejection fraction|EF]] is less than 55%.
 
[[Physical exercise|Low impact exercise]] (eg. [[swimming]]) should be advised. If [[myalgia]] presents, [[Physical exercise|physical activity]] should be reduced and [[myoglobinuria]] cheked out.


=== Surgery ===
* [[Heart transplantation|Cardiac transplantation]] may be requiered in patients with severe [[Dilated cardiomyopathy classification|dilated cardiomyopathy]].
[[Heart transplantation|Cardiac transplantation]] may be requiered in patients with severe [[Dilated cardiomyopathy classification|dilated cardiomyopathy]].


Severe or incapacitating [[scoliosis]] may be corrected with [[surgery]].
* Severe or incapacitating [[scoliosis]] may be corrected with [[surgery]].


=== Primary Prevention ===
=== Primary Prevention ===

Revision as of 20:01, 2 June 2020


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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Moises Romo, M.D.


Overview

Former "pseudohypertrophic muscular dystrophy", now Becker's muscular dystrophy, is a genetic neuromuscular condition characterized by slowly progresive weakness and atrophy of skeletal (mostly legs and pelvis) and cardiac muscles.

Historical Perspective

Pathophysiology

Clinical Features

Unlike Duchenne muscular dystrophy, Becker's muscular dystrophy (BMD) phenotype presents at a later age, widely variable onset from early childhood to late adulthood, most of them falling in puberty range. Most of the patients will requiere a wheelchair after age 16.

Clinical presentation Becker's muscular dystrophy include:

There is an abcense of fasciculations, and this finding may exclude BMD[2]

CNS is rarely afected in Becker's muscular dystrophy, for this reason, intelligence is usually spared.

Most of women are asymptomatic carriers, with very rare cases presenting the classic symptoms.

Differentiating Becker's muscular dystrophy from other Diseases

Becker's muscular dystrophy must be differentiated from other diseases that cause skelletal and cardiac muscle afection, such as:

Screening


Epidemiology and Demographics

  • The prevalence of Becker's muscular dystrophy is approximately 1-3 per 100,000 individuals.
  • The incidence of Becker's muscular dystrophy is approximately 3-6 per 100,000 male births worldwide.[4][5]

Age

Becker's muscular dystrophy is diagnosed in 85% of patients by age 25.

Gender

Becker's muscular dystrophy affects mostly men, women are carriers almost exclusively (except rare situation).

Race

  • Becker's muscular dystrophy usually affects individuals of the hispanic race.[6]
  • Asian individuals are less likely to develop Becker's muscular dystrophy.[7]

Risk Factors

Natural History, Complications and Prognosis


Diagnosis

The diagnosis of Becker's muscular dystrophy is made with a classic clinical presentation plus elevated CK, molecular genetic testing, or muscle biopsy.

Symptoms

Symptoms of Becker's muscular dystrophy may include the following:

Physical Examination

Patients with Becker's muscular dystrophy usually adapt a posture with shoulders held back, abdomen stuck out, and lumbar hyperlordosis.

Physical examination may be remarkable for:

Laboratory Findings

An elevated CK is typical in Becker's muscular dystrophy, with a peak around 10-15 years of age.[11]

Other laboratory finding consistent with Becker's muscular dystrophy may be:

Hystopathology

Histologic findings in Becker's muscular may be:

EMG

EMG in Becker's muscular dystrophy, may reveal myopathic motor units with or without muscle membrane instability.

Echocardiography

Echocardiogram should be done at the time of diagnosis.

Imaging Findings

There are no X-ray findings characteristic with with Becker's muscular dystrophy, but scoliosis may be found.

Treatment

Medical Therapy

Surgery

Primary Prevention

There are no primary preventive measures available for Becker's muscular dystrophy.

Secondary Prevention



References

{{Reflist|2}}

Template:Muscular Dystrophy it:Distrofia muscolare di Becker nl:Becker spierdystrofie no:Beckers muskeldystrofi fi:Beckerin lihasdystrofia


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