Clinical course of untreated cerebral cavernous malformations: A meta-analysis of individual patient data

Cerebral Cavernous Malformations Individual Patient Data Meta-analysis Collaborators

doi:10.1016/S1474-4422(15)00303-8

Clinical course of untreated cerebral cavernous malformations: A meta-analysis of individual patient data

Cerebral Cavernous Malformations Individual Patient Data Meta-analysis Collaborators

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Abstract

Background: Cerebral cavernous malformations (CCMs) can cause symptomatic intracranial haemorrhage (ICH), but the estimated risks are imprecise and predictors remain uncertain. We aimed to obtain precise estimates and predictors of the risk of ICH during untreated follow-up in an individual patient data meta-analysis. Methods: We invited investigators of published cohorts of people aged at least 16 years, identified by a systematic review of Ovid MEDLINE and Embase from inception to April 30, 2015, to provide individual patient data on clinical course from CCM diagnosis until first CCM treatment or last available follow-up. We used survival analysis to estimate the 5-year risk of symptomatic ICH due to CCMs (primary outcome), multivariable Cox regression to identify baseline predictors of outcome, and random-effects models to pool estimates in a meta-analysis. Findings: Among 1620 people in seven cohorts from six studies, 204 experienced ICH during 5197 person-years of follow-up (Kaplan-Meier estimated 5-year risk 15·8%, 95% CI 13·7-17·9). The primary outcome of ICH within 5 years of CCM diagnosis was associated with clinical presentation with ICH or new focal neurological deficit (FND) without brain imaging evidence of recent haemorrhage versus other modes of presentation (hazard ratio 5·6, 95% CI 3·2-9·7) and with brainstem CCM location versus other locations (4·4, 2·3-8·6), but age, sex, and CCM multiplicity did not add independent prognostic information. The 5-year estimated risk of ICH during untreated follow-up was 3·8% (95% CI 2·1-5·5) for 718 people with non-brainstem CCM presenting without ICH or FND, 8·0% (0·1-15·9) for 80 people with brainstem CCM presenting without ICH or FND, 18·4% (13·3-23·5) for 327 people with non-brainstem CCM presenting with ICH or FND, and 30·8% (26·3-35·2) for 495 people with brainstem CCM presenting with ICH or FND. Interpretation: Mode of clinical presentation and CCM location are independently associated with ICH within 5 years of CCM diagnosis. These findings can inform decisions about CCM treatment. Funding: UK Medical Research Council, Chief Scientist Office of the Scottish Government, and UK Stroke Association.

Original language	English (US)
Pages (from-to)	166-173
Number of pages	8
Journal	The Lancet Neurology
Volume	15
Issue number	2
DOIs	https://doi.org/10.1016/S1474-4422(15)00303-8
State	Published - Feb 1 2016

ASJC Scopus subject areas

Clinical Neurology

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10.1016/S1474-4422(15)00303-8

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@article{93d5150b7bb64a7ba856d3252c8b87a0,

title = "Clinical course of untreated cerebral cavernous malformations: A meta-analysis of individual patient data",

abstract = "Background: Cerebral cavernous malformations (CCMs) can cause symptomatic intracranial haemorrhage (ICH), but the estimated risks are imprecise and predictors remain uncertain. We aimed to obtain precise estimates and predictors of the risk of ICH during untreated follow-up in an individual patient data meta-analysis. Methods: We invited investigators of published cohorts of people aged at least 16 years, identified by a systematic review of Ovid MEDLINE and Embase from inception to April 30, 2015, to provide individual patient data on clinical course from CCM diagnosis until first CCM treatment or last available follow-up. We used survival analysis to estimate the 5-year risk of symptomatic ICH due to CCMs (primary outcome), multivariable Cox regression to identify baseline predictors of outcome, and random-effects models to pool estimates in a meta-analysis. Findings: Among 1620 people in seven cohorts from six studies, 204 experienced ICH during 5197 person-years of follow-up (Kaplan-Meier estimated 5-year risk 15·8%, 95% CI 13·7-17·9). The primary outcome of ICH within 5 years of CCM diagnosis was associated with clinical presentation with ICH or new focal neurological deficit (FND) without brain imaging evidence of recent haemorrhage versus other modes of presentation (hazard ratio 5·6, 95% CI 3·2-9·7) and with brainstem CCM location versus other locations (4·4, 2·3-8·6), but age, sex, and CCM multiplicity did not add independent prognostic information. The 5-year estimated risk of ICH during untreated follow-up was 3·8% (95% CI 2·1-5·5) for 718 people with non-brainstem CCM presenting without ICH or FND, 8·0% (0·1-15·9) for 80 people with brainstem CCM presenting without ICH or FND, 18·4% (13·3-23·5) for 327 people with non-brainstem CCM presenting with ICH or FND, and 30·8% (26·3-35·2) for 495 people with brainstem CCM presenting with ICH or FND. Interpretation: Mode of clinical presentation and CCM location are independently associated with ICH within 5 years of CCM diagnosis. These findings can inform decisions about CCM treatment. Funding: UK Medical Research Council, Chief Scientist Office of the Scottish Government, and UK Stroke Association.",

author = "{Cerebral Cavernous Malformations Individual Patient Data Meta-analysis Collaborators} and Horne, {Margaret A.} and Flemming, {Kelly D.} and Su, {I. Chang} and Christian Stapf and Jeon, {Jin Pyeong} and Da Li and Maxwell, {Susanne S.} and Philip White and Christianson, {Teresa J.} and Ronit Agid and Cho, {Won Sang} and Oh, {Chang Wan} and Zhen Wu and Zhang, {Jun Ting} and Kim, {Jeong Eun} and {ter Brugge}, Karel and Robert Willinsky and Brown, {R. D.} and Murray, {Gordon D.} and Salman, {Rustam Al Shahi} and S. Baird and Bhattacharya, {J. J.} and Counsell, {C. E.} and {St George}, {E. J.} and White, {P. M.} and V. Ritchie and Roberts, {R. C.} and Sellar, {R. J.} and Warlow, {C. P.} and Link, {M. J.} and M. Tymianski and Wallace, {M. C.} and D. Herv{\'e} and F. Riant and Schneble, {H. M.} and Chung, {Y. S.} and S. Oh and Ahn, {J. H.} and Son, {Y. J.} and Bang, {J. S.} and Kang, {H. S.} and Sohn, {C. H.} and Hao, {S. Y.} and Jia, {G. J.} and Zhang, {L. W.}",

note = "Funding Information: MAH reports grants from the Edinburgh Hub for Trials Methodology Research. GDM reports grants from the Medical Research Council, the Edinburgh Hub for Trials Methodology Research, the Chief Scientist Office of the Scottish Government, and the Stroke Association. KDF, I-CS, CS, JPJ, DL, SSM, PW, TJC, RA, W-SC, CWO, ZW, J-TZ, JEK, KtB, RW, RDB, and RA-SS declare no competing interests. Funding Information: This study was supported by the Medical Research Council (G84/5176, G108/613, G1002605) and the Edinburgh Hub for Trials Methodology Research (G0800803); the Chief Scientist Office of the Scottish Government (K/MRS/50/C2704 and CZB/4/35); and the Stroke Association (TSA04/01). We thank Rosemary Anderson, Aidan Hutchison, and all the people in the Scottish Audit of Intracranial Vascular Malformations; and Gail Nixon, clinical nurse coordinator, and Alex Kostynskyy, clinical research associate, of the Toronto Brain Vascular Malformation study group. Funding Information: This study was supported by the Medical Research Council (G84/5176, G108/613, G1002605) and the Edinburgh Hub for Trials Methodology Research (G0800803); the Chief Scientist Ofice of the Scottish Government (K/MRS/50/C2704 and CZB/4/35); and the Stroke Association (TSA04/01). We thank Rosemary Anderson, Aidan Hutchison, and all the people in the Scottish Audit of Intracranial Vascular Malformations; and Gail Nixon, clinical nurse coordinator, and Alex Kostynskyy, clinical research associate, of the Toronto Brain Vascular Malformation study group. Publisher Copyright: {\textcopyright} 2016 Horne et al. Open Access article distributed under the terms of CC BY.",

year = "2016",

month = feb,

day = "1",

doi = "10.1016/S1474-4422(15)00303-8",

language = "English (US)",

volume = "15",

pages = "166--173",

journal = "The Lancet Neurology",

issn = "1474-4422",

publisher = "Lancet Publishing Group",

number = "2",

}

TY - JOUR

T1 - Clinical course of untreated cerebral cavernous malformations

T2 - A meta-analysis of individual patient data

AU - Cerebral Cavernous Malformations Individual Patient Data Meta-analysis Collaborators

AU - Horne, Margaret A.

AU - Flemming, Kelly D.

AU - Su, I. Chang

AU - Stapf, Christian

AU - Jeon, Jin Pyeong

AU - Li, Da

AU - Maxwell, Susanne S.

AU - White, Philip

AU - Christianson, Teresa J.

AU - Agid, Ronit

AU - Cho, Won Sang

AU - Oh, Chang Wan

AU - Wu, Zhen

AU - Zhang, Jun Ting

AU - Kim, Jeong Eun

AU - ter Brugge, Karel

AU - Willinsky, Robert

AU - Brown, R. D.

AU - Murray, Gordon D.

AU - Salman, Rustam Al Shahi

AU - Baird, S.

AU - Bhattacharya, J. J.

AU - Counsell, C. E.

AU - St George, E. J.

AU - White, P. M.

AU - Ritchie, V.

AU - Roberts, R. C.

AU - Sellar, R. J.

AU - Warlow, C. P.

AU - Link, M. J.

AU - Tymianski, M.

AU - Wallace, M. C.

AU - Hervé, D.

AU - Riant, F.

AU - Schneble, H. M.

AU - Chung, Y. S.

AU - Oh, S.

AU - Ahn, J. H.

AU - Son, Y. J.

AU - Bang, J. S.

AU - Kang, H. S.

AU - Sohn, C. H.

AU - Hao, S. Y.

AU - Jia, G. J.

AU - Zhang, L. W.

N1 - Funding Information: MAH reports grants from the Edinburgh Hub for Trials Methodology Research. GDM reports grants from the Medical Research Council, the Edinburgh Hub for Trials Methodology Research, the Chief Scientist Office of the Scottish Government, and the Stroke Association. KDF, I-CS, CS, JPJ, DL, SSM, PW, TJC, RA, W-SC, CWO, ZW, J-TZ, JEK, KtB, RW, RDB, and RA-SS declare no competing interests. Funding Information: This study was supported by the Medical Research Council (G84/5176, G108/613, G1002605) and the Edinburgh Hub for Trials Methodology Research (G0800803); the Chief Scientist Office of the Scottish Government (K/MRS/50/C2704 and CZB/4/35); and the Stroke Association (TSA04/01). We thank Rosemary Anderson, Aidan Hutchison, and all the people in the Scottish Audit of Intracranial Vascular Malformations; and Gail Nixon, clinical nurse coordinator, and Alex Kostynskyy, clinical research associate, of the Toronto Brain Vascular Malformation study group. Funding Information: This study was supported by the Medical Research Council (G84/5176, G108/613, G1002605) and the Edinburgh Hub for Trials Methodology Research (G0800803); the Chief Scientist Ofice of the Scottish Government (K/MRS/50/C2704 and CZB/4/35); and the Stroke Association (TSA04/01). We thank Rosemary Anderson, Aidan Hutchison, and all the people in the Scottish Audit of Intracranial Vascular Malformations; and Gail Nixon, clinical nurse coordinator, and Alex Kostynskyy, clinical research associate, of the Toronto Brain Vascular Malformation study group. Publisher Copyright: © 2016 Horne et al. Open Access article distributed under the terms of CC BY.

PY - 2016/2/1

Y1 - 2016/2/1

N2 - Background: Cerebral cavernous malformations (CCMs) can cause symptomatic intracranial haemorrhage (ICH), but the estimated risks are imprecise and predictors remain uncertain. We aimed to obtain precise estimates and predictors of the risk of ICH during untreated follow-up in an individual patient data meta-analysis. Methods: We invited investigators of published cohorts of people aged at least 16 years, identified by a systematic review of Ovid MEDLINE and Embase from inception to April 30, 2015, to provide individual patient data on clinical course from CCM diagnosis until first CCM treatment or last available follow-up. We used survival analysis to estimate the 5-year risk of symptomatic ICH due to CCMs (primary outcome), multivariable Cox regression to identify baseline predictors of outcome, and random-effects models to pool estimates in a meta-analysis. Findings: Among 1620 people in seven cohorts from six studies, 204 experienced ICH during 5197 person-years of follow-up (Kaplan-Meier estimated 5-year risk 15·8%, 95% CI 13·7-17·9). The primary outcome of ICH within 5 years of CCM diagnosis was associated with clinical presentation with ICH or new focal neurological deficit (FND) without brain imaging evidence of recent haemorrhage versus other modes of presentation (hazard ratio 5·6, 95% CI 3·2-9·7) and with brainstem CCM location versus other locations (4·4, 2·3-8·6), but age, sex, and CCM multiplicity did not add independent prognostic information. The 5-year estimated risk of ICH during untreated follow-up was 3·8% (95% CI 2·1-5·5) for 718 people with non-brainstem CCM presenting without ICH or FND, 8·0% (0·1-15·9) for 80 people with brainstem CCM presenting without ICH or FND, 18·4% (13·3-23·5) for 327 people with non-brainstem CCM presenting with ICH or FND, and 30·8% (26·3-35·2) for 495 people with brainstem CCM presenting with ICH or FND. Interpretation: Mode of clinical presentation and CCM location are independently associated with ICH within 5 years of CCM diagnosis. These findings can inform decisions about CCM treatment. Funding: UK Medical Research Council, Chief Scientist Office of the Scottish Government, and UK Stroke Association.

AB - Background: Cerebral cavernous malformations (CCMs) can cause symptomatic intracranial haemorrhage (ICH), but the estimated risks are imprecise and predictors remain uncertain. We aimed to obtain precise estimates and predictors of the risk of ICH during untreated follow-up in an individual patient data meta-analysis. Methods: We invited investigators of published cohorts of people aged at least 16 years, identified by a systematic review of Ovid MEDLINE and Embase from inception to April 30, 2015, to provide individual patient data on clinical course from CCM diagnosis until first CCM treatment or last available follow-up. We used survival analysis to estimate the 5-year risk of symptomatic ICH due to CCMs (primary outcome), multivariable Cox regression to identify baseline predictors of outcome, and random-effects models to pool estimates in a meta-analysis. Findings: Among 1620 people in seven cohorts from six studies, 204 experienced ICH during 5197 person-years of follow-up (Kaplan-Meier estimated 5-year risk 15·8%, 95% CI 13·7-17·9). The primary outcome of ICH within 5 years of CCM diagnosis was associated with clinical presentation with ICH or new focal neurological deficit (FND) without brain imaging evidence of recent haemorrhage versus other modes of presentation (hazard ratio 5·6, 95% CI 3·2-9·7) and with brainstem CCM location versus other locations (4·4, 2·3-8·6), but age, sex, and CCM multiplicity did not add independent prognostic information. The 5-year estimated risk of ICH during untreated follow-up was 3·8% (95% CI 2·1-5·5) for 718 people with non-brainstem CCM presenting without ICH or FND, 8·0% (0·1-15·9) for 80 people with brainstem CCM presenting without ICH or FND, 18·4% (13·3-23·5) for 327 people with non-brainstem CCM presenting with ICH or FND, and 30·8% (26·3-35·2) for 495 people with brainstem CCM presenting with ICH or FND. Interpretation: Mode of clinical presentation and CCM location are independently associated with ICH within 5 years of CCM diagnosis. These findings can inform decisions about CCM treatment. Funding: UK Medical Research Council, Chief Scientist Office of the Scottish Government, and UK Stroke Association.

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SN - 1474-4422

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JO - The Lancet Neurology

JF - The Lancet Neurology

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ER -

Clinical course of untreated cerebral cavernous malformations: A meta-analysis of individual patient data

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