Approach to genetic analysis in the diagnosis of hereditary autoinflammatory syndromes

A. Simon; J.W.M. van der Meer; R. Veselý; U. Myrdal; K. Yoshimura; P. Duys; J.P.H. Drenth; A. Ahlin; C.G. Arvidsson; P. Betts; J.W.J. Bijlsma; R.H. van den Brink; L. Businco; C. Chapelon; C. J. Darroch; J. J. David; M. van Deuren; E. Drewe; E. Elias; T. Espanol; A. M. Farrell; T. Fiselier; E.V. Granowitz; H.J. Hasper; D. Jilek; D.C. Knockaert; M. Korppi; H.P.H. Kremer; T. W. Kuijpers; J. Louis; C.E.M. de Maat; J. Palmblad; P. Pohunek; R.J. Powell; J.J. Rasker; K. Riesbeck; U. Saatci; P.T.A. Schellekens; R.M. Scolozzi; C.D.A. Stehouwer; C.A.M. de Swart; K. Takada; R. Tamminga; T. Tribolet de Abreu; C.M.R. Weemaes

doi:10.1093/rheumatology/kei138

Approach to genetic analysis in the diagnosis of hereditary autoinflammatory syndromes

A. Simon^*, J.W.M. van der Meer, R. Veselý, U. Myrdal, K. Yoshimura, P. Duys, J.P.H. Drenth, A. Ahlin, C.G. Arvidsson, P. Betts, J.W.J. Bijlsma, R.H. van den Brink, L. Businco, C. Chapelon, C. J. Darroch, J. J. David, M. van Deuren, E. Drewe, E. Elias, T. EspanolA. M. Farrell, T. Fiselier, E.V. Granowitz, H.J. Hasper, D. Jilek, D.C. Knockaert, M. Korppi, H.P.H. Kremer, T. W. Kuijpers, J. Louis, C.E.M. de Maat, J. Palmblad, P. Pohunek, R.J. Powell, J.J. Rasker, K. Riesbeck, U. Saatci, P.T.A. Schellekens, R.M. Scolozzi, C.D.A. Stehouwer, C.A.M. de Swart, K. Takada, R. Tamminga, T. Tribolet de Abreu, C.M.R. Weemaes

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

Objective: Hereditary autoinflammatory syndromes are characterized by recurrent episodes of fever and inflammation. Seven subtypes have been described, caused by mutations in four different genes. Apart from a common phenotype of lifelong recurrent inflammatory attacks, all subtypes have distinct features and specific therapeutic options, which emphasizes the need for a specific diagnosis in each case. Our aim was to examine whether genetic screening would allow classification of previously unclassified patients, and whether individual patients suffering from an autoinflammatory syndrome carry additional mutations in one of the other autoinflammatory genes.

Methods: We included 60 patients with an unclassified autoinflammatory syndrome, 87 patients diagnosed with either hyper-IgD syndrome, familial Mediterranean fever (FMF) or tumour necrosis factor (TNF)-receptor-associated periodic syndrome and 50 healthy controls. Deoxyribonucleic acid samples were screened for the most prevalent mutations in the MEFV, TNFRSF1A, MVK and CIAS1 genes.

Results: We found only one possible diagnosis of FMF in the 60 previously unclassified patients. Two low-penetrance mutations were found in equal numbers in the groups of patients and controls.

Conclusions: Screening of highly prevalent mutations in known genes involved in these disorders does not yield additional relevant information. Differential diagnosis of hereditary autoinflammatory syndromes can be made by thorough clinical examination followed by targeted genetic analysis of the one or two most likely syndromes. High-prevalence low-penetrant mutations from autoinflammatory genes do not occur more frequently in patients with hereditary autoinflammatory syndromes compared with the general population.

Original language	English
Pages (from-to)	269-273
Number of pages	5
Journal	Rheumatology
Volume	45
Issue number	3
DOIs	https://doi.org/10.1093/rheumatology/kei138
Publication status	Published - 1 Mar 2006
Externally published	Yes

Keywords

CAPS
Cryopyrin
FMF
Hereditary autoinflammatory syndromes
HIDS
Mevalonate kinase
Periodic fever
Pyrin
TNFRSF1A
TRAPS

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Simon, A., van der Meer, J. W. M., Veselý, R., Myrdal, U., Yoshimura, K., Duys, P., Drenth, J. P. H., Ahlin, A., Arvidsson, C. G., Betts, P., Bijlsma, J. W. J., van den Brink, R. H., Businco, L., Chapelon, C., Darroch, C. J., David, J. J., van Deuren, M., Drewe, E., Elias, E., ... Weemaes, C. M. R. (2006). Approach to genetic analysis in the diagnosis of hereditary autoinflammatory syndromes. Rheumatology, 45(3), 269-273. https://doi.org/10.1093/rheumatology/kei138

@article{c98961beee2945faba5def4e4a713b82,

title = "Approach to genetic analysis in the diagnosis of hereditary autoinflammatory syndromes",

abstract = "Objective: Hereditary autoinflammatory syndromes are characterized by recurrent episodes of fever and inflammation. Seven subtypes have been described, caused by mutations in four different genes. Apart from a common phenotype of lifelong recurrent inflammatory attacks, all subtypes have distinct features and specific therapeutic options, which emphasizes the need for a specific diagnosis in each case. Our aim was to examine whether genetic screening would allow classification of previously unclassified patients, and whether individual patients suffering from an autoinflammatory syndrome carry additional mutations in one of the other autoinflammatory genes.Methods: We included 60 patients with an unclassified autoinflammatory syndrome, 87 patients diagnosed with either hyper-IgD syndrome, familial Mediterranean fever (FMF) or tumour necrosis factor (TNF)-receptor-associated periodic syndrome and 50 healthy controls. Deoxyribonucleic acid samples were screened for the most prevalent mutations in the MEFV, TNFRSF1A, MVK and CIAS1 genes.Results: We found only one possible diagnosis of FMF in the 60 previously unclassified patients. Two low-penetrance mutations were found in equal numbers in the groups of patients and controls.Conclusions: Screening of highly prevalent mutations in known genes involved in these disorders does not yield additional relevant information. Differential diagnosis of hereditary autoinflammatory syndromes can be made by thorough clinical examination followed by targeted genetic analysis of the one or two most likely syndromes. High-prevalence low-penetrant mutations from autoinflammatory genes do not occur more frequently in patients with hereditary autoinflammatory syndromes compared with the general population.",

keywords = "CAPS, Cryopyrin, FMF, Hereditary autoinflammatory syndromes, HIDS, Mevalonate kinase, Periodic fever, Pyrin, TNFRSF1A, TRAPS",

author = "A. Simon and {van der Meer}, J.W.M. and R. Vesel{\'y} and U. Myrdal and K. Yoshimura and P. Duys and J.P.H. Drenth and A. Ahlin and C.G. Arvidsson and P. Betts and J.W.J. Bijlsma and {van den Brink}, R.H. and L. Businco and C. Chapelon and Darroch, {C. J.} and David, {J. J.} and {van Deuren}, M. and E. Drewe and E. Elias and T. Espanol and Farrell, {A. M.} and T. Fiselier and E.V. Granowitz and H.J. Hasper and D. Jilek and D.C. Knockaert and M. Korppi and H.P.H. Kremer and Kuijpers, {T. W.} and J. Louis and {de Maat}, C.E.M. and J. Palmblad and P. Pohunek and R.J. Powell and J.J. Rasker and K. Riesbeck and U. Saatci and P.T.A. Schellekens and R.M. Scolozzi and C.D.A. Stehouwer and {de Swart}, C.A.M. and K. Takada and R. Tamminga and {Tribolet de Abreu}, T. and C.M.R. Weemaes",

year = "2006",

month = mar,

day = "1",

doi = "10.1093/rheumatology/kei138",

language = "English",

volume = "45",

pages = "269--273",

journal = "Rheumatology",

issn = "1462-0324",

publisher = "Oxford University Press",

number = "3",

}

Simon, A, van der Meer, JWM, Veselý, R, Myrdal, U, Yoshimura, K, Duys, P, Drenth, JPH, Ahlin, A, Arvidsson, CG, Betts, P, Bijlsma, JWJ, van den Brink, RH, Businco, L, Chapelon, C, Darroch, CJ, David, JJ, van Deuren, M, Drewe, E, Elias, E, Espanol, T, Farrell, AM, Fiselier, T, Granowitz, EV, Hasper, HJ, Jilek, D, Knockaert, DC, Korppi, M, Kremer, HPH, Kuijpers, TW, Louis, J, de Maat, CEM, Palmblad, J, Pohunek, P, Powell, RJ, Rasker, JJ, Riesbeck, K, Saatci, U, Schellekens, PTA, Scolozzi, RM, Stehouwer, CDA, de Swart, CAM, Takada, K, Tamminga, R, Tribolet de Abreu, T & Weemaes, CMR 2006, 'Approach to genetic analysis in the diagnosis of hereditary autoinflammatory syndromes', Rheumatology, vol. 45, no. 3, pp. 269-273. https://doi.org/10.1093/rheumatology/kei138

TY - JOUR

T1 - Approach to genetic analysis in the diagnosis of hereditary autoinflammatory syndromes

AU - Simon, A.

AU - van der Meer, J.W.M.

AU - Veselý, R.

AU - Myrdal, U.

AU - Yoshimura, K.

AU - Duys, P.

AU - Drenth, J.P.H.

AU - Ahlin, A.

AU - Arvidsson, C.G.

AU - Betts, P.

AU - Bijlsma, J.W.J.

AU - van den Brink, R.H.

AU - Businco, L.

AU - Chapelon, C.

AU - Darroch, C. J.

AU - David, J. J.

AU - van Deuren, M.

AU - Drewe, E.

AU - Elias, E.

AU - Espanol, T.

AU - Farrell, A. M.

AU - Fiselier, T.

AU - Granowitz, E.V.

AU - Hasper, H.J.

AU - Jilek, D.

AU - Knockaert, D.C.

AU - Korppi, M.

AU - Kremer, H.P.H.

AU - Kuijpers, T. W.

AU - Louis, J.

AU - de Maat, C.E.M.

AU - Palmblad, J.

AU - Pohunek, P.

AU - Powell, R.J.

AU - Rasker, J.J.

AU - Riesbeck, K.

AU - Saatci, U.

AU - Schellekens, P.T.A.

AU - Scolozzi, R.M.

AU - Stehouwer, C.D.A.

AU - de Swart, C.A.M.

AU - Takada, K.

AU - Tamminga, R.

AU - Tribolet de Abreu, T.

AU - Weemaes, C.M.R.

PY - 2006/3/1

Y1 - 2006/3/1

N2 - Objective: Hereditary autoinflammatory syndromes are characterized by recurrent episodes of fever and inflammation. Seven subtypes have been described, caused by mutations in four different genes. Apart from a common phenotype of lifelong recurrent inflammatory attacks, all subtypes have distinct features and specific therapeutic options, which emphasizes the need for a specific diagnosis in each case. Our aim was to examine whether genetic screening would allow classification of previously unclassified patients, and whether individual patients suffering from an autoinflammatory syndrome carry additional mutations in one of the other autoinflammatory genes.Methods: We included 60 patients with an unclassified autoinflammatory syndrome, 87 patients diagnosed with either hyper-IgD syndrome, familial Mediterranean fever (FMF) or tumour necrosis factor (TNF)-receptor-associated periodic syndrome and 50 healthy controls. Deoxyribonucleic acid samples were screened for the most prevalent mutations in the MEFV, TNFRSF1A, MVK and CIAS1 genes.Results: We found only one possible diagnosis of FMF in the 60 previously unclassified patients. Two low-penetrance mutations were found in equal numbers in the groups of patients and controls.Conclusions: Screening of highly prevalent mutations in known genes involved in these disorders does not yield additional relevant information. Differential diagnosis of hereditary autoinflammatory syndromes can be made by thorough clinical examination followed by targeted genetic analysis of the one or two most likely syndromes. High-prevalence low-penetrant mutations from autoinflammatory genes do not occur more frequently in patients with hereditary autoinflammatory syndromes compared with the general population.

AB - Objective: Hereditary autoinflammatory syndromes are characterized by recurrent episodes of fever and inflammation. Seven subtypes have been described, caused by mutations in four different genes. Apart from a common phenotype of lifelong recurrent inflammatory attacks, all subtypes have distinct features and specific therapeutic options, which emphasizes the need for a specific diagnosis in each case. Our aim was to examine whether genetic screening would allow classification of previously unclassified patients, and whether individual patients suffering from an autoinflammatory syndrome carry additional mutations in one of the other autoinflammatory genes.Methods: We included 60 patients with an unclassified autoinflammatory syndrome, 87 patients diagnosed with either hyper-IgD syndrome, familial Mediterranean fever (FMF) or tumour necrosis factor (TNF)-receptor-associated periodic syndrome and 50 healthy controls. Deoxyribonucleic acid samples were screened for the most prevalent mutations in the MEFV, TNFRSF1A, MVK and CIAS1 genes.Results: We found only one possible diagnosis of FMF in the 60 previously unclassified patients. Two low-penetrance mutations were found in equal numbers in the groups of patients and controls.Conclusions: Screening of highly prevalent mutations in known genes involved in these disorders does not yield additional relevant information. Differential diagnosis of hereditary autoinflammatory syndromes can be made by thorough clinical examination followed by targeted genetic analysis of the one or two most likely syndromes. High-prevalence low-penetrant mutations from autoinflammatory genes do not occur more frequently in patients with hereditary autoinflammatory syndromes compared with the general population.

KW - CAPS

KW - Cryopyrin

KW - FMF

KW - Hereditary autoinflammatory syndromes

KW - HIDS

KW - Mevalonate kinase

KW - Periodic fever

KW - Pyrin

KW - TNFRSF1A

KW - TRAPS

UR - http://www.scopus.com/inward/record.url?scp=33644867557&partnerID=8YFLogxK

U2 - 10.1093/rheumatology/kei138

DO - 10.1093/rheumatology/kei138

M3 - Article

C2 - 16234278

AN - SCOPUS:33644867557

SN - 1462-0324

VL - 45

SP - 269

EP - 273

JO - Rheumatology

JF - Rheumatology

IS - 3

ER -

Approach to genetic analysis in the diagnosis of hereditary autoinflammatory syndromes

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Keywords

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