HLA typing in acute optic neuritis: Relation to multiple sclerosis and magnetic resonance imaging findings

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Standard

HLA typing in acute optic neuritis : Relation to multiple sclerosis and magnetic resonance imaging findings. / Frederiksen, J L; Madsen, H O; Ryder, L P; Larsson, H B; Morling, N; Svejgaard, A.

In: Archives of Neurology, Vol. 54, No. 1, 1997, p. 76-80.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Frederiksen, JL, Madsen, HO, Ryder, LP, Larsson, HB, Morling, N & Svejgaard, A 1997, 'HLA typing in acute optic neuritis: Relation to multiple sclerosis and magnetic resonance imaging findings', Archives of Neurology, vol. 54, no. 1, pp. 76-80.

APA

Frederiksen, J. L., Madsen, H. O., Ryder, L. P., Larsson, H. B., Morling, N., & Svejgaard, A. (1997). HLA typing in acute optic neuritis: Relation to multiple sclerosis and magnetic resonance imaging findings. Archives of Neurology, 54(1), 76-80.

Vancouver

Frederiksen JL, Madsen HO, Ryder LP, Larsson HB, Morling N, Svejgaard A. HLA typing in acute optic neuritis: Relation to multiple sclerosis and magnetic resonance imaging findings. Archives of Neurology. 1997;54(1):76-80.

Author

Frederiksen, J L ; Madsen, H O ; Ryder, L P ; Larsson, H B ; Morling, N ; Svejgaard, A. / HLA typing in acute optic neuritis : Relation to multiple sclerosis and magnetic resonance imaging findings. In: Archives of Neurology. 1997 ; Vol. 54, No. 1. pp. 76-80.

Bibtex

@article{8e8e12f0e4b611deba73000ea68e967b,
title = "HLA typing in acute optic neuritis: Relation to multiple sclerosis and magnetic resonance imaging findings",
abstract = "OBJECTIVE: To study the association of brain magnetic resonance imaging (MRI) findings and HLA findings to clarify the relationship between monosymptomatic optic neuritis (ON) and ON as part of clinically definite multiple sclerosis (CDMS). DESIGN: Population-based cohort of patients with ON referred prospectively during 6 years by neurologists and ophthalmologists within 4 weeks of onset of ON. SETTING: Referral center in the general community of greater Copenhagen (Denmark) (population, 1.5 million). PATIENTS: A consecutive sample of 199 patients aged 12 to 59 years with ON (133 with idiopathic ON, 66 with ON + CDMS), ethnically matched with 192 healthy volunteers. MAIN OUTCOME MEASURES: Relation between the HLA-DR15, -DR17, -DQA-1B, and -DQB-1B polymorphisms as defined by restriction fragment length polymorphism analysis, and presence of plaques on T2-weighted brain MRI. RESULTS: The frequency of HLA-DR15 was significantly increased in patients with ON + CDMS (52%) and ON (47%) compared with control subjects (31%). The frequency of HLA-DR17 was almost equal in the ON + CDMS (18%), ON (23%), and control (23%) groups. The frequencies of HLA-DQA-1B (55% in ON + CDMS, 58% in ON) and HLA-DQB-1B (49% in ON + CDMS, 59% in ON) were significantly increased compared with control subjects (41%, HLA-DQA-1B; 37%, HLA-DQB-1B). Brain MRI was abnormal in 48 of 56 examined patients with ON + CDMS and in 64 of 120 examined patients with ON (P < .001). In contrast, the frequencies of HLA alleles did not differ between patients with and without demyelinating lesions. However, patients with ON and normal MRI findings did not show association with HLA-DR15. CONCLUSIONS: The frequencies of alleles were similar in patients with ON and ON + CDMS, confirming that they are not 2 immunogenetically distinct disease entities. The heterogeneity within the group of patients with ON suggests that the HLA-DR15 molecule is involved in susceptibility to initial demyelinating lesion formation.",
author = "Frederiksen, {J L} and Madsen, {H O} and Ryder, {L P} and Larsson, {H B} and N Morling and A Svejgaard",
note = "Keywords: Acute Disease; Adolescent; Adult; Alleles; Child; Female; HLA-DQ Antigens; HLA-DR Antigens; Humans; Immunophenotyping; Magnetic Resonance Imaging; Male; Middle Aged; Multiple Sclerosis; Optic Neuritis; Prospective Studies",
year = "1997",
language = "English",
volume = "54",
pages = "76--80",
journal = "JAMA Neurology",
issn = "2168-6149",
publisher = "The JAMA Network",
number = "1",

}

RIS

TY - JOUR

T1 - HLA typing in acute optic neuritis

T2 - Relation to multiple sclerosis and magnetic resonance imaging findings

AU - Frederiksen, J L

AU - Madsen, H O

AU - Ryder, L P

AU - Larsson, H B

AU - Morling, N

AU - Svejgaard, A

N1 - Keywords: Acute Disease; Adolescent; Adult; Alleles; Child; Female; HLA-DQ Antigens; HLA-DR Antigens; Humans; Immunophenotyping; Magnetic Resonance Imaging; Male; Middle Aged; Multiple Sclerosis; Optic Neuritis; Prospective Studies

PY - 1997

Y1 - 1997

N2 - OBJECTIVE: To study the association of brain magnetic resonance imaging (MRI) findings and HLA findings to clarify the relationship between monosymptomatic optic neuritis (ON) and ON as part of clinically definite multiple sclerosis (CDMS). DESIGN: Population-based cohort of patients with ON referred prospectively during 6 years by neurologists and ophthalmologists within 4 weeks of onset of ON. SETTING: Referral center in the general community of greater Copenhagen (Denmark) (population, 1.5 million). PATIENTS: A consecutive sample of 199 patients aged 12 to 59 years with ON (133 with idiopathic ON, 66 with ON + CDMS), ethnically matched with 192 healthy volunteers. MAIN OUTCOME MEASURES: Relation between the HLA-DR15, -DR17, -DQA-1B, and -DQB-1B polymorphisms as defined by restriction fragment length polymorphism analysis, and presence of plaques on T2-weighted brain MRI. RESULTS: The frequency of HLA-DR15 was significantly increased in patients with ON + CDMS (52%) and ON (47%) compared with control subjects (31%). The frequency of HLA-DR17 was almost equal in the ON + CDMS (18%), ON (23%), and control (23%) groups. The frequencies of HLA-DQA-1B (55% in ON + CDMS, 58% in ON) and HLA-DQB-1B (49% in ON + CDMS, 59% in ON) were significantly increased compared with control subjects (41%, HLA-DQA-1B; 37%, HLA-DQB-1B). Brain MRI was abnormal in 48 of 56 examined patients with ON + CDMS and in 64 of 120 examined patients with ON (P < .001). In contrast, the frequencies of HLA alleles did not differ between patients with and without demyelinating lesions. However, patients with ON and normal MRI findings did not show association with HLA-DR15. CONCLUSIONS: The frequencies of alleles were similar in patients with ON and ON + CDMS, confirming that they are not 2 immunogenetically distinct disease entities. The heterogeneity within the group of patients with ON suggests that the HLA-DR15 molecule is involved in susceptibility to initial demyelinating lesion formation.

AB - OBJECTIVE: To study the association of brain magnetic resonance imaging (MRI) findings and HLA findings to clarify the relationship between monosymptomatic optic neuritis (ON) and ON as part of clinically definite multiple sclerosis (CDMS). DESIGN: Population-based cohort of patients with ON referred prospectively during 6 years by neurologists and ophthalmologists within 4 weeks of onset of ON. SETTING: Referral center in the general community of greater Copenhagen (Denmark) (population, 1.5 million). PATIENTS: A consecutive sample of 199 patients aged 12 to 59 years with ON (133 with idiopathic ON, 66 with ON + CDMS), ethnically matched with 192 healthy volunteers. MAIN OUTCOME MEASURES: Relation between the HLA-DR15, -DR17, -DQA-1B, and -DQB-1B polymorphisms as defined by restriction fragment length polymorphism analysis, and presence of plaques on T2-weighted brain MRI. RESULTS: The frequency of HLA-DR15 was significantly increased in patients with ON + CDMS (52%) and ON (47%) compared with control subjects (31%). The frequency of HLA-DR17 was almost equal in the ON + CDMS (18%), ON (23%), and control (23%) groups. The frequencies of HLA-DQA-1B (55% in ON + CDMS, 58% in ON) and HLA-DQB-1B (49% in ON + CDMS, 59% in ON) were significantly increased compared with control subjects (41%, HLA-DQA-1B; 37%, HLA-DQB-1B). Brain MRI was abnormal in 48 of 56 examined patients with ON + CDMS and in 64 of 120 examined patients with ON (P < .001). In contrast, the frequencies of HLA alleles did not differ between patients with and without demyelinating lesions. However, patients with ON and normal MRI findings did not show association with HLA-DR15. CONCLUSIONS: The frequencies of alleles were similar in patients with ON and ON + CDMS, confirming that they are not 2 immunogenetically distinct disease entities. The heterogeneity within the group of patients with ON suggests that the HLA-DR15 molecule is involved in susceptibility to initial demyelinating lesion formation.

M3 - Journal article

C2 - 9006417

VL - 54

SP - 76

EP - 80

JO - JAMA Neurology

JF - JAMA Neurology

SN - 2168-6149

IS - 1

ER -

ID: 16186038