Osteogenesis imperfecta: Difference between revisions
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== Historical considerations == | == Historical considerations == | ||
The Osteogenesis Imperfecta (OI) was identified as a disease in the 17th century, however only in the 19<sup>th</sup> century was it recognized by the current designation. The system used today was presented by Sillence ''et al'', in 1979, which subdivides the disease in 4 groups depending on the severity and progression. | [[File:XrayOITypeV-Audult.jpg|250px|right]] | ||
'''The Osteogenesis Imperfecta''' (OI) was identified as a disease in the 17th century, however only in the 19<sup>th</sup> century was it recognized by the current designation. The system used today was presented by Sillence ''et al'', in 1979, which subdivides the disease in 4 groups depending on the severity and progression. | |||
== Characterization of disease == | == Characterization of disease == | ||
Osteogenesis Imperfecta is a hereditary disease caused by mutations in genes coding for [[collagen]], which leads to the formation of very fragile bones. Mutations that underlie this disease are transmitted to offspring in a [[Autosomal dominant inheritance|autosomal dominant]] inheritance (85-90% of [[Mutation|mutations]]). However, they are currently described 8 different types of this disease two of which (types VII and VIII) are inherited as [[Autosomal recessive inheritance|autosomal recessive]] form and do not include mutations in genes coding for collagen[[File:BonesCase-40,41-%26-42.jpg|250px|right]] | |||
Osteogenesis Imperfecta is a hereditary disease caused by mutations in genes coding for [[collagen]], which leads to the formation of very fragile bones. Mutations that underlie this disease are transmitted to offspring in a [[autosomal dominant]] inheritance (85-90% of mutations). However, they are currently described 8 different types of this disease two of which (types VII and VIII) are inherited as [[autosomal recessive]] form and do not include mutations in genes coding for collagen | |||
=== Prevalence and symptoms === | === Prevalence and symptoms === | ||
This | This genetic disorder affects between 6 to 7 individuals in 100.000 worldwide. Types I and IV are the most common forms of OI and affect 4 to 5 Individuals in 100000. | ||
Symptoms vary from person to person, even among individuals with the same type or within the same family. The main symptoms are blue [[ | Symptoms vary from person to person, even among individuals with the same type or within the same family. The main symptoms are blue [[Eye|scleras]], [[Dentiogenesis imperfecta|dentinogenesis imperfecta]], bone fragility, fragile ligament | ||
s and [[deafness]] in the case of the adult. | |||
=== Different types of OI === | === Different types of OI === | ||
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<small>AD- autosomal dominant; AR- Autosomal recessive</small> | <small>AD - autosomal dominant; AR- Autosomal recessive</small> | ||
== Diagnosis == | == Diagnosis == | ||
The first diagnostic approach is the study of differential family history and observation of patients for the identification of [[phenotype|phenotypic]] changes, in the latter case it may be necessary to use [[x- | The first diagnostic approach is the study of differential family history and observation of patients for the identification of [[phenotype|phenotypic]] changes, in the latter case it may be necessary to use [[x-rays]] to check the degree and type of fractures. For a more specific diagnosis, other types of tests such as [[skin]] [[biopsy]] are performed for analysis of structure and quantity of [[collagen]]. To confirm the differential diagnosis and prenatal diagnosis molecular tests have been carried out to detect the [[mutation]] and therefore be able to provide appropriate treatment to each patient. | ||
== Treatment == | == Treatment == | ||
The Osteogenesis Imperfecta is a disease that has no cure, however, these patients should practice some types of exercise and using, when appropriate, walking aids with the aim of improving their quality of life. In the most serious cases it is necessary to resort to surgeries and hormone treatments. The therapy that now offers a higher rate of success is the use of [[bisphosphonates]]. Although not a cure for this disease has the ability to increase bone mass and consequently reduce the number of fractures. | The Osteogenesis Imperfecta is a disease that has no cure, however, these patients should practice some types of exercise and using, when appropriate, walking aids with the aim of improving their quality of life. In the most serious cases it is necessary to resort to surgeries and [[hormone]] treatments. The therapy that now offers a higher rate of success is the use of [[bisphosphonates]]. Although not a cure for this disease has the ability to increase [[bone]] mass and consequently reduce the number of fractures. | ||
== Future prospects == | == Future prospects == | ||
The therapy used is currently restricted to the use of orthopedic equipment and bisphosphonates, both with limited success. The use of bisphosphonates improves patients' quality of life, however is not a cure for this disease. Future prospects are directed to the use of gene therapy or cell therapy. | The therapy used is currently restricted to the use of orthopedic equipment and bisphosphonates, both with limited success. The use of bisphosphonates improves patients' quality of life, however is not a cure for this disease. Future prospects are directed to the use of gene therapy or [[cell]] therapy. | ||
== Links == | == Links == | ||
* {{Cite | * {{Cite | ||
Revision as of 16:18, 19 December 2023
Historical considerations
The Osteogenesis Imperfecta (OI) was identified as a disease in the 17th century, however only in the 19th century was it recognized by the current designation. The system used today was presented by Sillence et al, in 1979, which subdivides the disease in 4 groups depending on the severity and progression.
Characterization of disease
Osteogenesis Imperfecta is a hereditary disease caused by mutations in genes coding for collagen, which leads to the formation of very fragile bones. Mutations that underlie this disease are transmitted to offspring in a autosomal dominant inheritance (85-90% of mutations). However, they are currently described 8 different types of this disease two of which (types VII and VIII) are inherited as autosomal recessive form and do not include mutations in genes coding for collagen
Prevalence and symptoms
This genetic disorder affects between 6 to 7 individuals in 100.000 worldwide. Types I and IV are the most common forms of OI and affect 4 to 5 Individuals in 100000. Symptoms vary from person to person, even among individuals with the same type or within the same family. The main symptoms are blue scleras, dentinogenesis imperfecta, bone fragility, fragile ligament
s and deafness in the case of the adult.
Different types of OI
8 different types are determined by the severity and progression of the disease:
| Type | Heredity | Severity | Fractures | Stature | Sclerotic | Deafness | Mutated Gene |
|---|---|---|---|---|---|---|---|
| I | AD | Light | Less than 100 | Normal | Blue | Yes (50%) | COL1A1 |
| II | AD | Very Severe | Multiple | Very Short | Dark Blue | - | COL1A1 or COL1A2 |
| III | AD | Severe | Multiple | Very Short | Blue | Yes | COL1A1 or COL1A2 |
| IV | AD | Moderate to Light | Multiple | Variable | White | Partial | COL1A1 or COL1A2 |
| V | AD | Moderate | Multiple | Variable | White | No | - |
| VI | AD | Moderate | Multiple | Short | White | No | - |
| VII | AR | Moderate | Multiple | Short | White | No | CRTAP |
| VIII | AR | Severe | Multiple | Very Short | White | Yes | LEPRE1 |
AD - autosomal dominant; AR- Autosomal recessive
Diagnosis
The first diagnostic approach is the study of differential family history and observation of patients for the identification of phenotypic changes, in the latter case it may be necessary to use x-rays to check the degree and type of fractures. For a more specific diagnosis, other types of tests such as skin biopsy are performed for analysis of structure and quantity of collagen. To confirm the differential diagnosis and prenatal diagnosis molecular tests have been carried out to detect the mutation and therefore be able to provide appropriate treatment to each patient.
Treatment
The Osteogenesis Imperfecta is a disease that has no cure, however, these patients should practice some types of exercise and using, when appropriate, walking aids with the aim of improving their quality of life. In the most serious cases it is necessary to resort to surgeries and hormone treatments. The therapy that now offers a higher rate of success is the use of bisphosphonates. Although not a cure for this disease has the ability to increase bone mass and consequently reduce the number of fractures.
Future prospects
The therapy used is currently restricted to the use of orthopedic equipment and bisphosphonates, both with limited success. The use of bisphosphonates improves patients' quality of life, however is not a cure for this disease. Future prospects are directed to the use of gene therapy or cell therapy.
Links
- STEINER, Robert D – PEPIN, Melanie G – BYERS, Peter H. Osteogenesis Imperfecta [online] . 2nd edition. 2005. Available from <http://www.ncbi.nlm.nih.gov/books/NBK1295/>. ISBN 20301472.
- GENETICS, Home References. Osteogenesis imperfecta [online]. The last revision November 2007, [cit. 2012-12-04]. <http://ghr.nlm.nih.gov/condition=osteogenesisimperfecta>.
Related Articles
- ROUGHLEY, PJ. , et al. Osteogenesis Imperfecta-Clinical and Molecular Diversity. European Cells and Materials. 2003, y. 2003, vol. 5, p. 41-47, ISSN 14562271.
- GLORIEUX, FH. , et al. Experience With Bisphosphonates in Osteogenesis Imperfecta. Pediatrics. 2007, y. 2007, vol. 119, p. 163-5, ISSN 17332237.
Other References
- National Institute of Health (NIH). Osteogenesis Imperfecta Overview [online]. [cit. 2012-12-04]. <http://www.niams.nih.gov/Health_Info/Bone/Osteogenesis_Imperfecta/overview.asp>.
