Aspirin and recurrent intracerebral hemorrhage in cerebral amyloid angiopathy

Biffi, Alessandro; Halpin, Amy; Towfighi, Amytis; Gilson, Aaron J.; Busl, Katharina M.; Rost, Natalia S.; Smith, Edward E.; Greenberg, Mark S.; Rosand, Jonathan; Viswanathan, Anand

doi:10.1212/wnl.0b013e3181eee40f

Cited by 296 publications

(293 citation statements)

References 29 publications

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“…3,5 A recent, large meta-analysis of case-control studies conclusively demonstrated that APOE e2 and e4 increase risk of ICH in the lobar brain regions. 6 An intriguing preliminary finding that emerged as well was an association between APOE e4, but not e2, and nonlobar ICH.…”

Section: Resultsmentioning

confidence: 99%

“…2 Previous studies demonstrated that survivors of ICH in the lobar brain regions are at higher risk of recurrence, and multiple predictors of recurrent lobar ICH have been identified. 3,4 Among these, the e2/e4 variants of the APOE gene are presumed to modify lobar ICH recurrence risk via their role in small vessel disease associated with cerebral amyloid angiopathy (CAA). 3,5 A recent, large meta-analysis of case-control studies conclusively demonstrated that APOE e2 and e4 increase risk of ICH in the lobar brain regions.…”

mentioning

confidence: 99%

“…3,4 Among these, the e2/e4 variants of the APOE gene are presumed to modify lobar ICH recurrence risk via their role in small vessel disease associated with cerebral amyloid angiopathy (CAA). 3,5 A recent, large meta-analysis of case-control studies conclusively demonstrated that APOE e2 and e4 increase risk of ICH in the lobar brain regions. 6 An intriguing preliminary finding that emerged as well was an association between APOE e4, but not e2, and nonlobar ICH.…”

mentioning

confidence: 99%

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APOE ε4 and lipid levels affect risk of recurrent nonlobar intracerebral hemorrhage

et al. 2015

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Objective: Genetic variants e2/e4 within the APOE gene are established risk factors for lobar intracerebral hemorrhage (ICH). Published preliminary data suggest a potential role for APOE e4 in risk of nonlobar ICH. We therefore investigated the role of APOE in recurrent nonlobar ICH, and sought to clarify whether effects of APOE on circulating lipids mediate this association.Methods: Three hundred sixty-three survivors of nonlobar ICH were followed prospectively for ICH recurrence, with APOE genotype determined at enrollment. All participants had clinical, demographic, and laboratory data captured at time of index ICH and during follow-up. Using a multivariate model, we performed association and interaction analyses of the relationships among APOE genotype, lipid levels, and recurrent nonlobar ICH. Results:We observed 29 nonlobar ICH recurrences among 363 survivors. APOE e4 was associated with recurrent nonlobar ICH (hazard ratio 5 1.31; 95% confidence interval 5 1.02-2.69; p 5 0.038) after adjustment for age/sex/ethnicity and cardiovascular risk factors. Increasing lowdensity lipoprotein (LDL) levels were associated with decreased risk of recurrent nonlobar ICH (p 5 0.027), as were decreasing HDL levels (p 5 0.046). LDL levels modified the association of APOE e4 with recurrent nonlobar ICH (mediation p , 0.05). No associations were identified between APOE e2 and recurrent nonlobar ICH.Conclusion: APOE e4 is associated with recurrent ICH in nonlobar brain regions, providing further evidence for its causal role in ICH unrelated to cerebral amyloid angiopathy. LDL levels modulated this effect, suggesting that circulating lipid levels may mediate a portion of the role of APOE e4 in nonlobar ICH. Neurology ® 2015;85:349-356 GLOSSARY CAA 5 cerebral amyloid angiopathy; CI 5 confidence interval; EMR 5 electronic medical record; HDL 5 high-density lipoprotein; HR 5 hazard ratio; ICH 5 intracerebral hemorrhage; IQR 5 interquartile range; LDL 5 low-density lipoprotein; TC 5 total cholesterol.Primary intracerebral hemorrhage (ICH) is the most lethal acute cerebrovascular disorder, its mortality rate ranging from 40% to 50% at 90 days from the initial bleeding event.1 Survivors are often burdened with substantial disability and face a high risk of recurrent ICH.2 Previous studies demonstrated that survivors of ICH in the lobar brain regions are at higher risk of recurrence, and multiple predictors of recurrent lobar ICH have been identified.3,4 Among these, the e2/e4 variants of the APOE gene are presumed to modify lobar ICH recurrence risk via their role in small vessel disease associated with cerebral amyloid angiopathy (CAA). 3,5 A recent, large meta-analysis of case-control studies conclusively demonstrated that APOE e2 and e4 increase risk of ICH in the lobar brain regions. 6 An intriguing preliminary finding that emerged as well was an association between APOE e4, but not e2, and nonlobar ICH.6 This finding warrants further exploration of its potential underlying biology, as nonlobar ICH is typically associate...

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Section: Resultsmentioning

confidence: 99%

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confidence: 99%

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confidence: 99%

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APOE ε4 and lipid levels affect risk of recurrent nonlobar intracerebral hemorrhage

et al. 2015

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“…It is likely that these abnormalities might render cortical-subcortical vessels more vulnerable to rupture and with less potential for tamponade compared to deep perforating arteries in the presence of excessive anticoagulation. 17,18 In addition, evidence supporting a link between CAA and OAC-ICH includes the demonstration that the APOE e2 allele, a known genetic risk factor of CAA-related lobar ICH, 19,20 is more common in warfarin-associated ICH than in control patients on warfarin without ICH, 8 and that individual cases of ICH following anticoagulation or coronary thrombolysis revealed advanced CAA on autopsy. 21,22 Our findings are in apparent disagreement with those derived from the PITCH study by DequatrePonchelle et al 12 who found no influence of OACs on the anatomical distribution of ICH but a significant effect of these compounds on the volume of deep brain hematomas.…”

Section: Statistical Analyses Differences Among the Treatment Groupsmentioning

confidence: 99%

Antithrombotic medications and the etiology of intracerebral hemorrhage

Pezzini

Grassi

Paciaroni³

et al. 2014

Neurology

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“…The microbleed burden could have significant implications for anti-platelet treatment in patients with CAA. 47 A subanalysis of the Perindopril protection against recurrent stroke study (PROGRESS) suggests that blood pressure control reduces the risk of CAA-related ICH and blood pressure lowering could be preventive against multiple causes of ICH. 48 Animal studies in mice suggest that AB immunotherapy could theoretically slow or stop the development of CAA; however, it remains unclear if these findings are applicable in humans.…”

Section: Prospects For Prevention and Treatmentmentioning

confidence: 99%

Update on Amyloid-associated Intracerebral Hemorrhage

Grysiewicz¹,

Gorelick²

2012

US Neurology

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Cerebral congophilic or amyloid angiopathy (CAA) is a clinicopathological entity that is considered a common cause of primary non-traumatic brain hemorrhage in the elderly. CAA is frequently associated with Alzheimers disease (AD) and has become a primary focus of scientific inquiry. The spectrum of intracerebral hemorrhage (ICH) that may occur in CAA includes: cerebral lobar hemorrhages, deep hemorrhages, purely subarachnoid and subdural hemorrhages and cerebral microbleeds. CAA is also associated with microinfarcts, leukoencephalopathy and superficial siderosis. This brief article will provide an update on the advances in our understanding of CAA-associated ICH with a focus on the following topics: neuropathology and mechanism of CAA-related hemorrhage; epidemiology, including genetic and other possible risk factors; clinical presentation; diagnosis, including newer imaging modalities; and prospects for prevention and treatment.

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Aspirin and recurrent intracerebral hemorrhage in cerebral amyloid angiopathy

Cited by 296 publications

References 29 publications

APOE ε4 and lipid levels affect risk of recurrent nonlobar intracerebral hemorrhage

APOE ε4 and lipid levels affect risk of recurrent nonlobar intracerebral hemorrhage

Antithrombotic medications and the etiology of intracerebral hemorrhage

Update on Amyloid-associated Intracerebral Hemorrhage

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