|
Investigation of potential copyright issue
Do not restore or edit the blanked content on this page until the issue is resolved by an administrator, copyright clerk or OTRS agent.
|
| If you have just labeled this page as a potential copyright issue, please follow the instructions for filing at the bottom of the box. |
|
The previous content of this page has been identified as posing a potential copyright issue, as a copy or modification of the text from the source(s) below, and is now listed on Wikipedia:Copyright problems:
- http://omim.org/entry/266920 (Duplication Detector report)
Unless the copyright status of the text on this page is clarified, it may be deleted one week after the time of its listing.
Temporarily, the original posting is still accessible for viewing in the page history.
|
Can you help resolve this issue?
If you hold the copyright to this text, you can license it in a manner that allows its use on Wikipedia. Click "Show" to see how.
- You must permit the use of your material under the terms of the Creative Commons Attribution-Sharealike 3.0 Unported License (CC-BY-SA) and the GNU Free Documentation License (GFDL) (unversioned, with no invariant sections, front-cover texts, or back-cover texts).
- Explain your intent to license the content on this article's discussion page
- To confirm your permission, you can either display a notice to this effect at the site of original publication or send an e-mail from an address associated with the original publication to permissions-en at wikimedia dot org or a postal letter to the Wikimedia Foundation. These messages must explicitly permit use under CC-BY-SA and the GFDL. See Wikipedia:Donating copyrighted materials.
- Note that articles on Wikipedia must be written from a neutral point of view and must be verifiable in published third-party sources; consider whether, copyright issues aside, your text is appropriate for inclusion in Wikipedia.
To demonstrate that this text is in the public domain, or is already under a license suitable for Wikipedia, click "Show".
Explain this on this article's discussion page, with reference to evidence. Wikipedia:Public domain and Wikipedia:Compatibly licensed may assist in determining the status.
Otherwise, you may write a new article without copyright-infringing material. Click "Show" to read where and how.
Your rewrite should be placed on this page, where it will be available for an administrator or clerk to review it at the end of the listing period. Follow this link to create the temporary subpage.
-
- Simply modifying copyrighted text is not sufficient to avoid copyright infringement—if the original copyright violation cannot be cleanly removed or the article reverted to a prior version, it is best to write the article from scratch. (See Wikipedia:Close paraphrasing.)
- For license compliance, any content used from the original article must be properly attributed; if you use content from the original, please leave a note at the top of your rewrite saying as much. You may duplicate non-infringing text that you had contributed yourself.
- It is always a good idea, if rewriting, to identify the point where the copyrighted content was imported to Wikipedia and to check to make sure that the contributor did not add content imported from other sources. When closing investigations, clerks and administrators may find other copyright problems than the one identified. If this material is in the proposed rewrite and cannot be easily removed, the rewrite may not be usable.
- State that you have created a rewrite on this article's discussion page.
|
| About importing text to Wikipedia
For more details on this topic, see Wikipedia:Copy-paste.
- Posting copyrighted material without the express permission of the copyright holder is unlawful and against Wikipedia policy.
- If you have express permission, this must be verified either by explicit release at the source or by e-mail or letter to the Wikimedia Foundation. See Wikipedia:Declaration of consent for all enquiries.
- Policy requires that we block those who repeatedly post copyrighted material without express permission.
|
Instructions for filing
If you have tagged the article for investigation, please complete the following steps:
|
| Conorenal syndrome |
| Classification and external resources |
| OMIM |
266920 |
Conorenal syndrome, also called Mainzer-Saldino syndrome or Saldino-Mainzer disease, is a collection of medical conditions that seem to have a common genetic cause.
This syndrome was originally characterized during 1970 by Mainzer[1], et al., in a paper published in the American Journal of Medicine. In 1979, Giedion [2] summarized the cases of 8 individuals under the age of 11 years with chronic renal failure and phalangeal cone-shaped epiphyses of the hands (in other words, the epiphyses of the fingers were cone-shaped and protrude into the metaphysis), coining the term 'conorenal syndrome.' Half of Giedion's patients had retinitis pigmentosa (also called RP, a progressive degeneration of the retina which affects night vision and peripheral vision) and 25% had ataxia (an inability to coordinate muscular movements). Giedion reported nephronophthisis (a kidney disease with cysts in the tubules) in his patients; however, neither biopsy material nor clinical course was available to confirm that diagnosis. Mendley et al. (1995) extended the delineation of the conorenal syndrome to include renal histopathologic (features that can be identified in the laboratory) and clinical features of a primarily glomerular disorder (a kidney disorder involving the glomeruli, or clusters of blood vessels that act as filters in the kidney) [3]. A recent article by Beals and Weleber (2007) also noted that a majority of patients also have small capital femoral epiphyses (the very tops of the femur where it hits the hip socket ) and/or mild abnormalities of the promixal femoral metaphysis[4].
Mechanism
While it is not fully characterized as such, yet, conorenal syndrome seems to be an uncharacterized form of ciliopathy. A ciliopathy is a disease that affects the cilia (sensing cells within the body).
The link to ciliar problems as a cause for Nephronopthisis and similar Kidney diseases is relatively new. Watnick and Germino[5] note that NPHP1 and NPHP4 encode for the proteins nephrocystin and nephrocystin-4 (nephroretinin). These have been shown to interact in a series of cell-cell and cell-matrix signaling proteins. NPHP2 has been also shown to have possible links to the function of the primary renal cilium and to control of the cell cycle (Otto).[6] Otto further found that nephrocystin, inversin (INVS) and nephroretinin colocalize in the primary cilia of cultured renal epithelia cells [6]. One interesting connection is that primary cilia in renal cells may perform a sensing function which maintains the renal tubules. The loss of cystoproteins may lead to dysregulated growth.
The link to a ciliar disfunction in the Retinal degenerative diseases also comes from Otto. Like the described Kidney diseases, Retinitis Pigmentosa is a disease where the ciliar cells (Rods and Cones) fail to thrive. In a study of patients with a disease similar to Conorenal (renal-retinal Senior-Loken) the authors state "We show that nephrocystin-5, RPGR and calmodulin can be coimmniprecipitated from retinal extracts, and that these proteins localize to connecting cilia of photoreceptors and to primary cilia of renal epithelial cells. Our studies emphasize the central role of ciliary discfunction in the pathogenisis of renal-retinal Senior Loken Syndrome." In other words, there is a common link between certain kidney diseases and some forms of RP and it is through the something related to a problem in the cilia cells. This may be a problem in the cells themselves, or with something that keeps them alive and healthy.
Outcomes
When originally characterized by Giedion, there was a relatively high mortality rate due to untreated kidney failure (end stage renal disease - ESRD). The remarkable improvements in kidney transplantation have reduced the mortality of Conorenal Syndrome substantially if not eliminated it entirely. Most diagnosis of the disease occurs when children present with kidney failure - usually between the ages of 10 and 14. There are no known cures for the syndrome and management of the symptoms seems to be the typical approach.
Genetics
The exact gene loci has not been characterized.
- NPHP3: Olbrich, et al.[7], found mutations in the NPHP3 gene that cause nepnroonophthisis and a version of Retinitis Pigmentosa called Lebers Congenital Amaurosis (Senior Loken Syndrome) and hepatic syndrome. Their research leads them to conclude "Our findings suggest that the NPHP genes (NPHP1, NPHP3, NPHP4) involved in the pathogenesis of recessive cystic kidney disease also belong to a common pathway in the primary cilium of kidney cells."
- NPHP5: Otto, et al. found through positional cloning that NPHP5 (IQCB1) is the most frequent cause of a disease very similar to Conorenal Syndrome (renal-retinal Senior-Loken Syndrome).
References
- ^ Mainzer F, Saldino RM, Ozonoff MB, Minagi H (October 1970). "Familial nephropathy associatdd with retinitis pigmentosa, cerebellar ataxia and skeletal abnormalities". Am. J. Med. 49 (4): 556–62. doi:10.1016/S0002-9343(70)80051-1. PMID 4991086.
- ^ Giedion A (February 1979). "Phalangeal cone shaped epiphysis of the hands (PhCSEH) and chronic renal disease--the conorenal syndromes". Pediatr Radiol 8 (1): 32–8. doi:10.1007/BF00973675. PMID 431989.
- ^ Mendley SR, Poznanski AK, Spargo BH, Langman CB (May 1995). "Hereditary sclerosing glomerulopathy in the conorenal syndrome". Am. J. Kidney Dis. 25 (5): 792–7. doi:10.1016/0272-6386(95)90556-1. PMID 7747734. http://linkinghub.elsevier.com/retrieve/pii/S0272638695001090.
- ^ Beals RK, Weleber RG (October 2007). "Conorenal dysplasia: a syndrome of cone-shaped epiphysis, renal disease in childhood, retinitis pigmentosa and abnormality of the proximal femur". Am. J. Med. Genet. A 143A (20): 2444–7. doi:10.1002/ajmg.a.31948. PMID 17853467.
- ^ Watnick T, Germino G (August 2003). "From cilia to cyst" (PDF). Nat. Genet. 34 (4): 355–6. doi:10.1038/ng0803-355. PMID 12923538. http://www.nature.com/ng/journal/v34/n4/pdf/ng0803-355.pdf.
- ^ a b Otto EA, Loeys B, Khanna H, et al. (March 2005). "Nephrocystin-5, a ciliary IQ domain protein, is mutated in Senior-Loken syndrome and interacts with RPGR and calmodulin". Nat. Genet. 37 (3): 282–8. doi:10.1038/ng1520. PMID 15723066. http://www.nature.com/ng/journal/v37/n3/full/ng1520.html.
- ^ Olbrich H, Fliegauf M, Hoefele J, et al. (August 2003). "Mutations in a novel gene, NPHP3, cause adolescent nephronophthisis, tapeto-retinal degeneration and hepatic fibrosis". Nat. Genet. 34 (4): 455–9. doi:10.1038/ng1216. PMID 12872122. http://www.nature.com/ng/journal/v34/n4/full/ng1216.html.
