Английская Википедия:Ciliopathy

Материал из Онлайн справочника
Версия от 02:46, 19 февраля 2024; EducationBot (обсуждение | вклад) (Новая страница: «{{Английская Википедия/Панель перехода}} {{short description|Genetic disease resulting in abnormal formation or function of cilia}} {{cs1 config|name-list-style=vanc|display-authors=6}} {{Infobox medical condition (new) | name = Ciliopathy | synonyms = | image = Eukaryotic cilium diagram en.svg | alt = | caption = Eukaryotic cilium | pronounce = | field = | geneR...»)
(разн.) ← Предыдущая версия | Текущая версия (разн.) | Следующая версия → (разн.)
Перейти к навигацииПерейти к поиску

Шаблон:Short description Шаблон:Cs1 config Шаблон:Infobox medical condition (new)

A ciliopathy is any genetic disorder that affects the cellular cilia or the cilia anchoring structures, the basal bodies,[1] or ciliary function.[2] Primary cilia are important in guiding the process of development, so abnormal ciliary function while an embryo is developing can lead to a set of malformations that can occur regardless of the particular genetic problem.[3] The similarity of the clinical features of these developmental disorders means that they form a recognizable cluster of syndromes, loosely attributed to abnormal ciliary function and hence called ciliopathies. Regardless of the actual genetic cause, it is clustering of a set of characteristic physiological features which define whether a syndrome is a ciliopathy.

Although ciliopathies are usually considered to involve proteins that localize to motile and/or immotile (primary) cilia or centrosomes, it is possible for ciliopathies to be associated with unexpected proteins such as XPNPEP3, which localizes to mitochondria but is believed to affect ciliary function through proteolytic cleavage of ciliary proteins.[4]

Significant advances in understanding the importance of cilia were made in the mid-1990s. For example, the discovery of the role of cilia in embryonic development, identification of ciliary defects in genetic disorders such as Polycystic kidney disease, Bardet–Biedl syndrome and Primary ciliary dyskinesia.[5][6] However, the physiological role that this organelle plays in most tissues remains elusive. Additional studies of how ciliary dysfunction can lead to such severe disease and developmental pathologies is still a subject of current research.[7]

Signs and symptoms

A wide variety of symptoms are potential clinical features of ciliopathy. The signs most exclusive to a ciliopathy, in descending order of exclusivity, are:[8]Шаблон:Rp

A case with polycystic ovary syndrome, multiple subcutaneous cysts, renal function impairment, Caroli disease and liver cirrhosis due to ciliopathy has been described.[9]

Phenotypes sometimes associated with ciliopathies can include:[8]

Pathophysiology

"In effect, the motile cilium is a nanomachine composed of perhaps over 600 proteins in molecular complexes, many of which also function independently as nanomachines." Cilia "function as mechano- or chemosensors and as a cellular global positioning system to detect changes in the surrounding environment." For example, ciliary signaling plays a role in the initiation of cellular replacement after cell damage.[11]

In addition to this sensory role mediating specific signaling cues, cilia play "a secretory role in which a soluble protein is released to have an effect downstream of the fluid flow" in epithelial cells, and can of course mediate fluid flow directly in the case of motile cilia.[1] Primary cilia in the retina play a role in transferring nourishment to the non-vascularized rod and cone cells from the pigment epithelial vascularized cells several micrometres behind the surface of the retina.

Signal transduction pathways involved include the Hedgehog signaling pathway and the Wnt signaling pathway.[12]

Dysfunctional cilia can lead to:

In organisms of normal health, cilia are critical for:[15]

Genetics

"Just as different genes can contribute to similar diseases, so the same genes and families of genes can play a part in a range of different diseases." For example, in just two of the diseases caused by malfunctioning cilia, Meckel–Gruber syndrome and Bardet–Biedl syndrome, patients who carry mutations in genes associated with both diseases "have unique symptoms that are not seen in either condition alone." The genes linked to the two different conditions "interact with each other during development." Systems biologists are endeavoring to define functional modules containing multiple genes and then look at disorders whose phenotypes fit into such modules.[16]

A particular phenotype can overlap "considerably with several conditions (ciliopathies) in which primary cilia are also implicated in pathogenicity. One emerging aspect is the wide spectrum of ciliopathy gene mutations found within different diseases."[10]

Additionally, clinical presentations of patients with identical mutation can differ, suggesting the role of genetic modifiers.[17]

As of 2017, 187 ciliopathy associated genes have been confirmed, while the roles of further 241 candidate genes are still being investigated.[18]

A common way to identify ciliopathies such as ADPKD and ARPKD which have known genetic causes, is through linkage analysis direct mutation screening.[19] Other techniques, such as gene panels and whole-exome sequencing and whole genome sequencing can also be used to provide distinct advantages.[19][20] Gene panels analyse specific sets of genes and can be more comprehensive than single gene or direct mutation screening. Whole-exome/genome sequencing can screen for heterozygous carriers, and detect novel/rare variations.[19][21]

Mutations in the PKD1 and PKD2 genes which encode for polycystin-1 and polycistin-2 respectively are known to be causes of ADPKD, a ciliopathy that presents with the formation and growth of cysts in the kidneys, leading to renal failure.[22]

List of ciliopathies

"The phenotypic parameters that define a ciliopathy may be used to both recognize the cellular basis of a number of genetic disorders and to facilitate the diagnosis and treatment of some diseases of unknown" cause.[8]

Known ciliopathies

Condition OMIM Gene(s) Systems/organs affected
Alström syndrome[8][1] Шаблон:OMIM ALMS1
Asphyxiating thoracic dysplasia (Jeune syndrome)[8][23] Шаблон:OMIM
Bardet–Biedl syndrome[8][7][10] Шаблон:OMIM BBS1, BBS2, ARL6, BBS4, BBS5, MKKS, BBS7, TTC8, BBS9, BBS10, TRIM32, BBS12
Ellis–van Creveld syndrome[23] Шаблон:OMIM EVC, EVC2
Joubert syndrome[8][10] Шаблон:OMIM INPP5E, TMEM216, AHI1, NPHP1, CEP290, TMEM67, RPGRIP1L, ARL13B, CC2D2A, BRCC3 Brain
Leber congenital amaurosis[23] Шаблон:OMIM GUCY2D, RPE65
McKusick–Kaufman syndrome[23] Шаблон:OMIM MKKS
Meckel–Gruber syndrome[8][10][24] Шаблон:OMIM MKS1, TMEM67, TMEM216, CEP290, RPGRIP1L, CC2D2A Liver, heart, bone
Nephronophthisis[8][7][10] Шаблон:OMIM NPHP1, INVS, NPHP3, NPHP4, IQCB1, CEP290, GLIS2, RPGRIP1L Kidney
Orofaciodigital syndrome 1[1][7] Шаблон:OMIM OFD1
Polycystic kidney disease[8][7] (ADPKD and ARPKD)[25] Шаблон:OMIM PKD1, PKD2, PKHD1 Kidney
Primary ciliary dyskinesia (Kartagener syndrome)[8] Шаблон:OMIM DNAI1, DNAH5, TXNDC3, DNAH11, DNAI2, KTU, RSPH4A, RSPH9, LRRC50
Senior–Løken syndrome[7] Шаблон:OMIM NPHP1, NPHP4, IQCB1, CEP290, SDCCAG8 Eye
Sensenbrenner syndrome (cranioectodermal dysplasia)[23] Шаблон:OMIM IFT122
Short rib–polydactyly syndrome[23] Шаблон:OMIM DYNC2H1
? ? IFT88 Novel form of congenital anosmia, reported in 2012[26]

Likely ciliopathies

Condition OMIM Gene(s) Systems/organs affected
Acrocallosal syndrome[23] Шаблон:OMIM KIF7, GLI3
Acromelic frontonasal dysostosis[23] Шаблон:OMIM ZSWIM6
Arima syndrome[23] Шаблон:OMIM
Biemond syndrome[23] Шаблон:OMIM
COACH syndrome[23] Шаблон:OMIM TMEM67, CC2D2A, RPGRIP1L
Conorenal syndrome[27][23] Шаблон:OMIM
Greig cephalopolysyndactyly syndrome[23] Шаблон:OMIM GLI3
Hydrolethalus syndrome[23] Шаблон:OMIM HYLS1
Johanson–Blizzard syndrome[23] Шаблон:OMIM UBR1
Mohr syndrome (oral-facial-digital syndrome type 2)[23] Шаблон:OMIM
Neu–Laxova syndrome[23] Шаблон:OMIM PHGDH, PSAT1, PSPH
Opitz G/BBB syndrome[23] Шаблон:OMIM MID1
Pallister–Hall syndrome[23] Шаблон:OMIM GLI3
Papillorenal syndrome[23] Шаблон:OMIM PAX2
Renal–hepatic–pancreatic dysplasia[23] Шаблон:OMIM NPHP3
Varadi–Papp syndrome (oral-facial-digital syndrome type 6)[23] Шаблон:OMIM

Possible ciliopathies

Condition OMIM Gene(s) Systems/organs affected
Acrofacial dysostosis[23]
Acrofrontofacionasal dysostosis 2[23] Шаблон:OMIM
Adams–Oliver syndrome[23] Шаблон:OMIM ARHGAP31, DOCK6, RBPJ, EOGT, NOTCH1, DLL4
Asplenia with cardiovascular anomalies (Ivemark syndrome)[23] Шаблон:OMIM
Autosomal recessive spastic paraplegia[23]
Barakat syndrome (HDR syndrome)[23] Шаблон:OMIM GATA3
Basal cell nevus syndrome[23] Шаблон:OMIM PTCH1, PTCH2, SUFU
Branchio‐oculo‐facial syndrome[23] Шаблон:OMIM TFAP2A
C syndrome (Opitz trigonocephaly)[23] Шаблон:OMIM CD96
Carpenter syndrome[23] Шаблон:OMIM RAB23
Cephaloskeletal dysplasia (microcephalic osteodysplastic primordial dwarfism type 1)[23] Шаблон:OMIM RNU4ATAC
Cerebrofaciothoracic dysplasia[23] Шаблон:OMIM TMCO1
Cerebrofrontofacial syndrome (Baraitser–Winter syndrome)[23] Шаблон:OMIM ACTB
Cerebrooculonasal syndrome[23] Шаблон:OMIM
Autosomal recessive spastic ataxia of Charlevoix-Saguenay[23] Шаблон:OMIM SACS
Chondrodysplasia punctata 2[23] Шаблон:OMIM EBP
Choroideremia[23] Шаблон:OMIM CHM
Chudley–McCullough syndrome[23] Шаблон:OMIM GPSM2
C‐like syndrome[23] Шаблон:OMIM ASXL1
Coffin–Siris syndrome[23] Шаблон:OMIM ARID1B, SOX11, ARID2
Cohen syndrome[23] Шаблон:OMIM VPS13B
Craniofrontonasal dysplasia[23] Шаблон:OMIM EFNB1
Dysgnathia complex[23] Шаблон:OMIM
Ectrodactyly–ectodermal dysplasia–cleft syndrome type 1[23] Шаблон:OMIM
Endocrine–cerebroosteodysplasia syndrome[23] Шаблон:OMIM ICK
Focal dermal hypoplasia[23] Шаблон:OMIM PORCN
Frontonasal dysplasia[23] Шаблон:OMIM ALX3, ALX4, ALX1
Fryns microphthalmia syndrome[23] Шаблон:OMIM
Fryns syndrome[23] Шаблон:OMIM
Genitopatellar syndrome[23] Шаблон:OMIM KAT6B
Hemifacial microsomia[23] Шаблон:OMIM
Hypothalamic hamartomas[23] Шаблон:OMIM
Johnson neuroectodermal syndrome[23] Шаблон:OMIM
Juvenile myoclonic epilepsy[28] Шаблон:OMIM
Kabuki syndrome[23] Шаблон:OMIM KMT2D, KDM6A
Kallmann syndrome[23] Шаблон:OMIM ANOS1
Lenz–Majewski hyperostotic dwarfism[23] Шаблон:OMIM PTDSS1
Lissencephaly 3[23] Шаблон:OMIM TUBA1A
Marden–Walker syndrome[8][23] Шаблон:OMIM PIEZO2
MASA syndrome[23] Шаблон:OMIM L1CAM
Microhydranencephaly[23] Шаблон:OMIM NDE1
Mowat–Wilson syndrome[23] Шаблон:OMIM ZEB2
NDH syndrome[23] Шаблон:OMIM GLIS3
Oculoauriculofrontonasal syndrome[23] Шаблон:OMIM
Oculocerebrocutaneous syndrome[23] Шаблон:OMIM
Oculodentodigital dysplasia[23] Шаблон:OMIM GJA1
Optiz–Kaveggia syndrome[23] Шаблон:OMIM MED12
Otopalatodigital syndrome 2[23] Шаблон:OMIM FLNA
Periventricular heterotopia X‐linked[23] Шаблон:OMIM FLNA
Perlman syndrome[23] Шаблон:OMIM DIS3L2
Pitt–Hopkins syndrome[23] Шаблон:OMIM TCF4
Polycystic liver disease[8] Шаблон:OMIM
Proteus syndrome[23] Шаблон:OMIM AKT1
Pseudotrisomy 13[23] Шаблон:OMIM
Retinal cone dystrophy 1[23] Шаблон:OMIM
Some forms of retinitis pigmentosa[8][29][23] Шаблон:OMIM
Robinow syndrome[23] Шаблон:OMIM ROR2
Rubinstein–Taybi syndrome[23] Шаблон:OMIM CREBBP
Sakoda complex[23] Шаблон:OMIM
Schinzel–Giedion syndrome[23] Шаблон:OMIM SETBP1
Split-hand/foot malformation 3[23] Шаблон:OMIM
Spondyloepiphyseal dysplasia congenita[23] Шаблон:OMIM COL2A1
Thanatophoric dysplasia[23] Шаблон:OMIM FGFR3
Townes–Brocks syndrome[23] Шаблон:OMIM SALL1, DACT1
Tuberous sclerosis[23] Шаблон:OMIM TSC1, TSC2
VATER association[23] Шаблон:OMIM
Ven den Ende–Gupta syndrome[23] Шаблон:OMIM SCARF2
Visceral heterotaxy[23] Шаблон:OMIM
Walker–Warburg syndrome[23] Шаблон:OMIM
Warburg Micro syndrome[23] Шаблон:OMIM RAB3GAP1
X‐linked congenital hydrocephalus[23] Шаблон:OMIM L1CAM
X‐linked lissencephaly[23] Шаблон:OMIM DCX
Young–Simpson syndrome[23] Шаблон:OMIM KAT6B

History

In 1674-1677, the Dutch scientist Antonie van Leeuwenhoek changed humanity's perspective on the world with his discovery of "animalcules" in rainwater, along with their tiny appendages known as cilia today. It was marked as the first recorded observation of single-celled organisms and their locomotive structures.[30]

In the late 19th century, Karl Ernst von Baer's groundbreaking work in embryonic development laid the foundation for modern developmental biology.[31] Through meticulous observations, von Baer provided invaluable insights into tissue and organ formation during development, including the early stages of embryogenesis and the development of cilia-bearing tissues.[32] While von Baer may not have fully appreciated the significance of cilia at the time, his observations likely included their presence in embryonic tissues. Cilia - crucial for cell signaling, tissue development, and left-right asymmetry, are now recognized as ancient organelles with essential roles in development.[33] Von Baer's concept of embryonic recapitulation, despite refinement, underscores the evolutionary conservation of developmental processes, including ciliary function. Today, von Baer's legacy inspires ongoing research into embryology and developmental biology, particularly in understanding ciliary biology and its relevance to ciliopathies, where defects in ciliary structure or function lead to developmental disorder.[34]

Although non-motile or primary cilia were first described in 1898, they were largely ignored by biologists. However, microscopists continued to document their presence in the cells of most vertebrate organisms. The primary cilium was long considered—with few exceptions—to be a largely useless evolutionary vestige, a vestigial organelle. Recent research has revealed that cilia are essential to many of the body's organs.[35] These primary cilia play important roles in chemosensation, mechanosensation, and thermosensation. Cilia may thus be "viewed as sensory cellular antennae that coordinate a large number of cellular signaling pathways, sometimes coupling the signaling to ciliary motility or alternatively to cell division and differentiation."[11]

Recent advances in mammalian genetic research have made possible the understanding of a molecular basis for a number of dysfunctional mechanisms in both motile and primary cilia structures of the cell.[36] A number of critical developmental signaling pathways essential to cellular development have been discovered. These are principally but not exclusively found in the non-motile or primary cilia. A number of common observable characteristics of mammalian genetic disorders and diseases are caused by ciliary dysgenesis and dysfunction. Once identified, these characteristics thus describe a set of hallmarks of a ciliopathy.[8]

Cilia have recently been implicated in a wide variety of human genetic diseases by "the discovery that numerous proteins involved in mammalian disease localize to the basal bodies and cilia." For example, in just a single area of human disease physiology, cystic renal disease, cilia-related genes and proteins have been identified to have causal effect in polycystic kidney disease, nephronophthisis, Senior–Løken syndrome type 5, orofaciodigital syndrome type 1 and Bardet–Biedl syndrome.[7]

References

Шаблон:Reflist

External links

Шаблон:Medical resources

Шаблон:Other genetic disorders by mechanism

  1. 1,0 1,1 1,2 1,3 1,4 1,5 1,6 Шаблон:Cite journal
  2. Шаблон:Cite journal
  3. Шаблон:Cite journal
  4. Шаблон:Cite journal
  5. Шаблон:Cite book
  6. Шаблон:Cite book
  7. 7,0 7,1 7,2 7,3 7,4 7,5 7,6 Шаблон:Cite journal
  8. 8,00 8,01 8,02 8,03 8,04 8,05 8,06 8,07 8,08 8,09 8,10 8,11 8,12 8,13 8,14 Шаблон:Cite journal
  9. Tan K, Liu P, Pang L, Yang W, Hou F (2018) A human ciliopathy with polycystic ovarian syndrome and multiple subcutaneous cysts: A rare case report. Medicine (Baltimore) 97(50)
  10. 10,0 10,1 10,2 10,3 10,4 10,5 Шаблон:Cite book
  11. 11,0 11,1 Шаблон:Cite journal
  12. Шаблон:Cite journal
  13. 13,0 13,1 13,2 13,3 Шаблон:Cite web
  14. Шаблон:Cite journal
  15. of organs The Ciliary Proteome Шаблон:Webarchive, Ciliaproteome V3.0 - Home Page, accessed 2010-06-11.
  16. Шаблон:Cite journal
  17. Шаблон:Cite journal
  18. Шаблон:Cite journal
  19. 19,0 19,1 19,2 Шаблон:Cite journal
  20. Шаблон:Cite web
  21. Шаблон:Cite journal
  22. Шаблон:Cite web
  23. 23,00 23,01 23,02 23,03 23,04 23,05 23,06 23,07 23,08 23,09 23,10 23,11 23,12 23,13 23,14 23,15 23,16 23,17 23,18 23,19 23,20 23,21 23,22 23,23 23,24 23,25 23,26 23,27 23,28 23,29 23,30 23,31 23,32 23,33 23,34 23,35 23,36 23,37 23,38 23,39 23,40 23,41 23,42 23,43 23,44 23,45 23,46 23,47 23,48 23,49 23,50 23,51 23,52 23,53 23,54 23,55 23,56 23,57 23,58 23,59 23,60 23,61 23,62 23,63 23,64 23,65 23,66 23,67 23,68 23,69 23,70 23,71 23,72 23,73 23,74 23,75 23,76 23,77 23,78 23,79 23,80 23,81 23,82 23,83 23,84 23,85 23,86 23,87 23,88 23,89 23,90 23,91 23,92 Шаблон:Cite journal
  24. Шаблон:Cite web
  25. Шаблон:Cite journal
  26. Gene therapy rescues cilia defects and restores olfactory function in a mammalian ciliopathy model
  27. Шаблон:Cite journal
  28. Шаблон:Cite journal
  29. Шаблон:Cite journal
  30. Шаблон:Cite journal
  31. Шаблон:Cite journal
  32. Шаблон:Cite journal
  33. Шаблон:Cite journal
  34. Шаблон:Cite journal
  35. Шаблон:Cite journal
  36. Шаблон:Cite journal