Papillorenal syndrome risk factors: Difference between revisions

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{{CMG}} {{AE}} {{Shivam Singla}}
==Overview==
==Overview==
The pathophysiology and the risk factors for responsible for the development of Renal coloboma syndrome is mainly genetic and related to the expression of PAX 2 gene. So the genetic inheritance is the main risk factor and this genetic syndrome keeps on clustering in the future generations. The environmental risk factors that impacts the pregnancy like alcohol and some drugs may contribute to the development of Renal-coloboma syndrome. In conclusion it arises from the abnormal development of organs like kidney and eyes during the pregnancy period. The abnormal development of eyes usually happens in the third trimester during that time the eyes are formed. The abnormalities usually happen when there in failure of optic disc closure. It usually depends on which specific part or areas of optic fissure fails to close.
==Risk factors==
The pathophysiology and the risk factors for responsible for the development of Renal coloboma syndrome is mainly genetic and related to the expression of PAX 2 gene. So the genetic inheritance is the main risk factor and this genetic syndrome keeps on clustering in the future generations. The environmental risk factors that impacts the pregnancy like alcohol and some drugs may contribute to the development of Renal-coloboma syndrome. In conclusion it arises from the abnormal development of organs like kidney and eyes during the pregnancy period. The abnormal development of eyes usually happens in the third trimester during that time the eyes are formed. The abnormalities usually happen when there in failure of optic disc closure. It usually depends on which specific part or areas of optic fissure fails to close.
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{{Papillorenal syndrome}}
{{Papillorenal syndrome}}
The [[pathophysiology]] and the [[risk factors]] responsible for the development of [[Renal-coloboma syndrome]] is mainly [[genetic]] and related to the expression of [[PAX 2]] [[gene]]. So the [[genetic]] [[inheritance]] is the main [[risk factor]] or the important determinant in the causation of [[Renal-coloboma syndrome]]. This [[genetic]] syndrome keeps on clustering in the future generations.


Coloboma or keyhole pupil might occurs all of sudden at its own during the pregnancy or it may be acquired. Some cases reported that even isolated coloboma are passed from one generation to another.
The [[environmental]] [[risk factors]] that impact the [[pregnancy]] like [[alcohol]] and some [[drugs]] may also contribute to the development of [[Renal-coloboma syndrome]]. In conclusion, [[RCS]] leads to the abnormal development of organs like [[kidney]] and [[eyes]] during the [[pregnancy period]]. The abnormal development of [[eyes]] usually happens in the third trimester during that time the [[eyes]] are formed. The abnormalities usually occur due to the impairment in the closure of the [[optic disc]]. It usually depends on which specific part or areas of [[optic fissure]] fails to close.


Prenatal care and diagnostic evaluation is possible for the cases where there is high index of suspicion or if there is clear cut family history of PAX2 gene mutation running in the family. This Renal-coloboma syndrome usually presents in autosomal dominant pattern with variations and complications due to other associated genetic manipulations like variable expression, genetic mosaicism and/or incomplete penetrance.
==Risk factors==
 
The [[pathophysiology]] and the risk factors responsible for the development of [[Renal-coloboma syndrome]] is mainly [[genetic]] and related to the expression of [[PAX2]]<ref name="pmid11297491">{{cite journal |vauthors=Parsa CF, Silva ED, Sundin OH, Goldberg MF, De Jong MR, Sunness JS, Zeimer R, Hunter DG |title=Redefining papillorenal syndrome: an underdiagnosed cause of ocular and renal morbidity |journal=Ophthalmology |volume=108 |issue=4 |pages=738–49 |date=April 2001 |pmid=11297491 |doi=10.1016/s0161-6420(00)00661-8 |url=}}</ref><ref name="pmid21654726">{{cite journal |vauthors=Schimmenti LA |title=Renal coloboma syndrome |journal=Eur. J. Hum. Genet. |volume=19 |issue=12 |pages=1207–12 |date=December 2011 |pmid=21654726 |pmc=3230355 |doi=10.1038/ejhg.2011.102 |url=}}</ref> [[gene]]. So the [[genetic inheritance]] is the main [[risk factor]] and this [[genetic syndrome]] keeps on clustering in the future generations. The [[environmental]] [[risk factors]] that impact the [[pregnancy]] like [[alcohol]] and some [[drugs]] may contribute to the development of [[Renal-coloboma syndrome]]. In conclusion, RCS leads to the abnormal development of [[organs]] like [[kidney]] and [[eyes]] during the [[pregnancy]] period. The abnormal development of [[eyes]] usually happens in the [[third trimester]] during that time the [[eyes]] are formed. The abnormalities usually happen when there is a failure of [[optic disc]] closure. It usually depends on which specific part or areas of optic fissure fails to close.
The eyes in the fetus develops during the first 3 months. Choroidal fissure forms the eye. This usually closes by the seventh week of pregnancy and failure of closure of this results in the development of coloboma. Usually affects one eye but at point seen affecting both eyes as well. There are different types of coloboma based on the structural and functional tissue of eye affected.  
 
Lens coloboma- The missing part is the lens piece
 
Eyelid coloboma- The missing tissue here is part of upper or lower eyelids.
 
Optic nerve coloboma- Optic nerve is affected that results in the impairment of vision.


Uveal coloboma- If the coloboma affects the iris then it is given a special name called Cat-eye appearance.
[[Coloboma]]<ref name="pmid26571382">{{cite journal |vauthors=Okumura T, Furuichi K, Higashide T, Sakurai M, Hashimoto S, Shinozaki Y, Hara A, Iwata Y, Sakai N, Sugiyama K, Kaneko S, Wada T |title=Association of PAX2 and Other Gene Mutations with the Clinical Manifestations of Renal Coloboma Syndrome |journal=PLoS ONE |volume=10 |issue=11 |pages=e0142843 |date=2015 |pmid=26571382 |pmc=4646464 |doi=10.1371/journal.pone.0142843 |url=}}</ref> or keyhole [[pupil]] might occurs all of sudden at its own during the pregnancy or it may be acquired. Some cases reported that even isolated coloboma is passed from one generation to another.


Chorio-retinal coloboma- Retina is the missing part in this case.
Prenatal care and diagnostic evaluation are possible for the cases where there is a high index of suspicion or if there is a clear cut family history of [[PAX2|PAX2 gen]]<nowiki/>e mutation running in the family. This [[Renal-coloboma syndrome]] usually presents in [[autosomal dominant]] pattern with variations and complications due to other associated genetic manipulations like variable expression, [[Mosaicism|genetic mosaicism]] and/or [[incomplete penetrance]].


Macular coloboma- The development of macula is abnormal in this case.
The eyes in the fetus develop during the first 3 months. Choroidal fissure forms the eye. This usually closes by the seventh week of pregnancy and failure of closure of this results in the development of [[coloboma]]. Usually affects one eye but at point seen affecting both eyes as well. There are different types of coloboma based on the structural and functional tissue of the eye affected.  


'''Lens coloboma'''- The missing part is the [[Lens|lens piece]]


'''Eyelid coloboma'''- The missing tissue here is part of the upper or lower eyelids.


'''Optic nerve coloboma'''- [[Optic nerve|Optic nerv]]<nowiki/>e is affected that results in the impairment of vision.


h.
'''Uveal coloboma'''- If the coloboma affects the iris then it is given a special name called [[Cat-eye syndrome|Cat-eye appearance]].


'''Chorio-retinal coloboma'''- [[Retina]] is the missing part in this case.


The wide association between urinary tract malformations and dysplastic kidneys, known as CAKUT (Congenital Anomalies of the Kidney and Urinary Tract), could be caused by a single disorder of the embryonic development of the kidney and urinary tract. These complex patterns of development are under genetic control. A positive family history strongly suggests a genetic origin of these conditions. Linkage studies show an extreme genetic heterogenicity and an important phenotypic and clinical variability of the same mutation. Some urinary tract malformations have been investigated in the context of clinical syndromes. The renal-coloboma syndrome is an autosomal dominant human disease, secondary to mutation of the PAX2 transcription factor, characterized by optic nerve coloboma, renal anomalies and vesicoureteral reflux. However, most of the urinary tract anomalies can occur in isolation. Studies have shown the association of hereditary hydronephrosis with HLA antigens on chromosome 6 and the association of VUR with the mutations in a locus of chromosome 1. The higher frequency and severity of some uropathies in the male gender may be explained by a linkage-disequilibrium phenomenon or a X-linked transmission pattern. For example, the mutations in the AGTR2 gene on chromosome X were observed in animal models but not yet confirmed in human subjects. Finally, the ACE gene polymorphism is associated with a higher incidence of congenital hypo-dysplastic kidneys and represents a significant risk factor for the development of progressive
'''Macular coloboma'''- The development of macula is abnormal in this case.


==References==
==References==

Latest revision as of 14:42, 10 September 2020

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Shivam Singla, M.D.[2]

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The pathophysiology and the risk factors responsible for the development of Renal-coloboma syndrome is mainly genetic and related to the expression of PAX 2 gene. So the genetic inheritance is the main risk factor or the important determinant in the causation of Renal-coloboma syndrome. This genetic syndrome keeps on clustering in the future generations.

The environmental risk factors that impact the pregnancy like alcohol and some drugs may also contribute to the development of Renal-coloboma syndrome. In conclusion, RCS leads to the abnormal development of organs like kidney and eyes during the pregnancy period. The abnormal development of eyes usually happens in the third trimester during that time the eyes are formed. The abnormalities usually occur due to the impairment in the closure of the optic disc. It usually depends on which specific part or areas of optic fissure fails to close.

Risk factors

The pathophysiology and the risk factors responsible for the development of Renal-coloboma syndrome is mainly genetic and related to the expression of PAX2[1][2] gene. So the genetic inheritance is the main risk factor and this genetic syndrome keeps on clustering in the future generations. The environmental risk factors that impact the pregnancy like alcohol and some drugs may contribute to the development of Renal-coloboma syndrome. In conclusion, RCS leads to the abnormal development of organs like kidney and eyes during the pregnancy period. The abnormal development of eyes usually happens in the third trimester during that time the eyes are formed. The abnormalities usually happen when there is a failure of optic disc closure. It usually depends on which specific part or areas of optic fissure fails to close.

Coloboma[3] or keyhole pupil might occurs all of sudden at its own during the pregnancy or it may be acquired. Some cases reported that even isolated coloboma is passed from one generation to another.

Prenatal care and diagnostic evaluation are possible for the cases where there is a high index of suspicion or if there is a clear cut family history of PAX2 gene mutation running in the family. This Renal-coloboma syndrome usually presents in autosomal dominant pattern with variations and complications due to other associated genetic manipulations like variable expression, genetic mosaicism and/or incomplete penetrance.

The eyes in the fetus develop during the first 3 months. Choroidal fissure forms the eye. This usually closes by the seventh week of pregnancy and failure of closure of this results in the development of coloboma. Usually affects one eye but at point seen affecting both eyes as well. There are different types of coloboma based on the structural and functional tissue of the eye affected.

Lens coloboma- The missing part is the lens piece

Eyelid coloboma- The missing tissue here is part of the upper or lower eyelids.

Optic nerve coloboma- Optic nerve is affected that results in the impairment of vision.

Uveal coloboma- If the coloboma affects the iris then it is given a special name called Cat-eye appearance.

Chorio-retinal coloboma- Retina is the missing part in this case.

Macular coloboma- The development of macula is abnormal in this case.

References

  1. Parsa CF, Silva ED, Sundin OH, Goldberg MF, De Jong MR, Sunness JS, Zeimer R, Hunter DG (April 2001). "Redefining papillorenal syndrome: an underdiagnosed cause of ocular and renal morbidity". Ophthalmology. 108 (4): 738–49. doi:10.1016/s0161-6420(00)00661-8. PMID 11297491.
  2. Schimmenti LA (December 2011). "Renal coloboma syndrome". Eur. J. Hum. Genet. 19 (12): 1207–12. doi:10.1038/ejhg.2011.102. PMC 3230355. PMID 21654726.
  3. Okumura T, Furuichi K, Higashide T, Sakurai M, Hashimoto S, Shinozaki Y, Hara A, Iwata Y, Sakai N, Sugiyama K, Kaneko S, Wada T (2015). "Association of PAX2 and Other Gene Mutations with the Clinical Manifestations of Renal Coloboma Syndrome". PLoS ONE. 10 (11): e0142843. doi:10.1371/journal.pone.0142843. PMC 4646464. PMID 26571382.

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