Update on Genetics of Stroke and Cerebrovascular Disease 2005
2006; Lippincott Williams & Wilkins; Volume: 37; Issue: 2 Linguagem: Inglês
10.1161/01.str.0000200449.58684.8a
ISSN1524-4628
AutoresHugh S. Markus, Mark J. Alberts,
Tópico(s)Cerebrovascular and genetic disorders
ResumoHomeStrokeVol. 37, No. 2Update on Genetics of Stroke and Cerebrovascular Disease 2005 Free AccessReview ArticlePDF/EPUBAboutView PDFView EPUBSections ToolsAdd to favoritesDownload citationsTrack citationsPermissions ShareShare onFacebookTwitterLinked InMendeleyReddit Jump toFree AccessReview ArticlePDF/EPUBUpdate on Genetics of Stroke and Cerebrovascular Disease 2005 Hugh S. Markus and Mark J. Alberts Hugh S. MarkusHugh S. Markus From the Clinical Neuroscience (H.S.M.), St Georges, University of London, London, UK; and the Department of Neurology (M.J.A.), Northwestern University, Feinberg School of Medicine, Chicago, IL. and Mark J. AlbertsMark J. Alberts From the Clinical Neuroscience (H.S.M.), St Georges, University of London, London, UK; and the Department of Neurology (M.J.A.), Northwestern University, Feinberg School of Medicine, Chicago, IL. Originally published12 Jan 2006https://doi.org/10.1161/01.STR.0000200449.58684.8aStroke. 2006;37:288–290Other version(s) of this articleYou are viewing the most recent version of this article. Previous versions: January 12, 2006: Previous Version 1 Over the past 2 years this update reported the identification by the Icelandic Decode group of 2 novel genes associated with ischemic stroke: phosphodiesterase 4D gene (PDE4D) and 5-Lipoxygenase activating protein (ALOX5AP).1,2 These putative associations have been with specific haplotypes of each gene, but no disease-specific mutations in either gene have been identified.PDE4D, a cyclic nucleotide phosphodiesterase, selectively degrades second messenger cAMP (cAMP). Reduced cAMP levels are associated with increased smooth muscle cell proliferation and migration, key events in atherosclerosis, making an association with stroke pathophysiologically plausible. Consistent with this, the initial association was reported only with large artery and cardioembolic stroke subtypes.2 Studies over the last year attempting to replicate this association have produced diverse results. In a UK population no overall association was found with ischemic stroke, but possible associations were identified with cardioembolic and large artery stroke.3 An American study reported an association with ischemic stroke, particularly large artery stroke.4 In contrast, no association was found in a German stroke cohort,5 or a Swedish stroke cohort aged <75 years.6 A linkage study from a second Swedish population confirmed linkage to 5q12,6 but no linkage study could be found in an American population.4 No association was found with carotid intima-media thickness,3 suggesting PDE4D does not exert its effects via accelerating early atherosclerosis.ALOX5AP codes for 5-lipoxygenase activating protein which is essential for conversion of arachadonic acid to leukotriene A4, a process catabolized by 5-lipooxygenase. LTA4 is converted into LTB4, which plays a crucial role in leukocyte chemotaxis and inflammatory responses, key processes in atherosclerosis. This pathway was also implicated in a separate study reporting an association between 5-lipooxygenase itself and carotid intima-media thickness.7 A number of groups have attempted to replicate the association of ischemic stroke with the ALOX5AP gene. The DeCode group replicated the association in a Scottish stroke population.8 A case control study from Germany reported a weak association with an ALOX5AP polymorphism.5 In American populations, no association was found in a case control study, or linkage to this chromosomal region in an affected sibling pair study.3There are a number of reasonable explanations for such disparate results. There might be significant genetic heterogeneity for ischemic stroke, thereby producing different results in different study populations. Population-specific genetic ancestral commonalities (and differences) might account for divergent results among patients in different countries. Lastly, random chance might produce spurious positive associations in some populations and studies, but not others. Further large studies in multiple populations are required to better define the biologic importance of these specific genes in ischemic stroke.There continues to be a large number of other candidate gene studies published over the last year reporting associations between polymorphisms in a wide variety of genes and stroke. Many of these have produced inconclusive results because of methodological problems and inadequate sample size. A recent review of these issues was published in Stroke and provides guidelines for future studies.9 An important consideration is the heterogeneity of stroke and potential for genetic variants to selectively predispose to particular stroke subtypes. The need for large well-phenotyped populations, ideally aged <65 to 70 years in whom the genetic component seems to be stronger, is becoming recognized, leading to a number of multicenter stroke DNA banks being established.Most stroke association studies have looked at single or a few single nucleotide polymorphisms (SNPs). In many cases, groups of nearby SNPs segregate as 1 genetic trait, with relatively little recombination or variation among such markers. A grouping of such SNPs is referred to as a haplotype. In 2005 a large multinational effort produced a haplotype map of the entire human genome (the HapMap Project), which involved analyzing over 1 000 000 SNPs in 269 individuals from Nigeria, China, Europe, Japan, and the United States.10 In some cases, the haplotypes demonstrated significant stability and lack of recombination. For example, 1 region that had 36 SNPs might have given rise to as many as 236 different haplotypes, yet only 7 different haplotypes were seen among 120 parental chromosomes. On the other hand, there are many well-defined 'hot-spots' for recombination throughout the genome that are well defined by the HapMap. In combination, these markers and related databases are powerful tools for gene association studies aimed at identifying genes involved in many complex human disorders.An emerging theme in stroke and cardiovascular disease genetics is the importance of gene-environment interaction.11 A number of conventional risk factors, such as smoking and obesity, may act via promoting a proinflammatory response. Polymorphisms in genes affecting the inflammatory response were reported as weak risk factors for carotid atherosclerosis in the population as a whole, but interacted strongly with these conventional proinflammatory risk factors.12 Such interactions need to be taken into account in planning future stroke genetic studies.An alternative approach is to take a monogenic disease in which stroke is a known complication and look at which other genes modify clinical presentation, as performed in an impressive study in sickle cell disease. Sickle cell disease results from homozygosity of a unique β-globin mutation. It shows marked phenotypic heterogeneity with stroke only affecting 6% to 8% of individuals. Using Bayesian networks 108 SNPs in 39 candidate genes in 1398 individuals with sickle cell disease were analyzed.13 Thirty-one SNPs in 12 genes were found to interact with fetal hemoglobin to modulate the risk of stroke, including 3 genes in the transforming growth factor-β pathway and P-selectin (SELP). A model developed predicted the occurrence of stroke in a second population with 98.2% accuracy.CADASIL is a rare but classic example of a monogenic type of inherited stroke syndrome. Further insights in the pathophysiology of this autosomal dominant disorder have been provided by studies in transgenic mice expressing typical CADASIL mutations. These mice showed early abnormal cerebral autoregulation, suggesting a causal role for alterations in vessel reactivity in disease pathogenesis.14 As in sickle cell disease, there is marked variation in the CADASIL phenotype, which is not explained by the mutation site. Evidence is emerging that the coexistence of conventional cardiovascular risk factors, such as smoking, may hasten disease progression.15The genetics of aneurysmal subarachnoid hemorrhage (SAH) and intracranial aneurysms (IAs) is an area of continuing study. One population-based study of patients with SAH in Scotland reported a 4.7% lifetime risk of SAH in first degree relatives, which tended to increase if 2 first degree relatives were affected.16 A number of genetic linkage studies have reported positive findings for various regions and putative candidate genes,17–19 although causative mutations have yet to be described (see Table). New Genetic Linkage for SAH and AneurysmsPhenotypeChromosomeLOD ScoreCommentsReference*These scores are nonparametric LOD scores. LOD indicates logarithm of odds.IACH17cen3.00*Japanese families15IACH 19q132.15*Japanese families15IAXp222.16*Japanese families15IA1p34.3-p36.134.2Dominant pattern16IACH2p133.55Dutch family17Cerebral cavernous malformations (CCM) are inherited in many cases. Three loci for familial CCMs have been previously identified, and the causative genes for CCM1 and CCM2 have been identified and the mutations have been well characterized. The causative gene for CCM3 was recently shown to be PDCD10 (programmed cell death10).20 A variety of mutations in PDCD10 have been observed to cosegregate with CCM, including nonsense, splicing, and frame shift. These findings suggest that apoptosis may play an important role in vascular morphogenesis and remodelling.In summary, 2005 has been a year of significant advances along many different fronts in understanding the genetics of ischemic and hemorrhagic stroke. As new resources such as the HapMap database become more widely used, we are hopeful that new genes will be identified and that previous associations will be definitively proven or disproven. This will allow the field to advance and identify causative genes and mutations that will eventually lead to improved prevention and treatment strategies.FootnotesCorrespondence to Hugh S. Markus, Centre for Clinical Neuroscience, St Georges, University of London, Cranmer Terrace, London SW17 ORW. E-mail [email protected]References1 Gretarsdottir S, Thorleifsson G, Reynisdottir ST, Manolescu A, Jonsdottir S, Jonsdottir T, Gudmundsdottir T, Bjarnadottir SM, Einarsson OB, Gudjonsdottir HM, Hawkins M, Gudmundsson G, Gudmundsdottir H, Andrason H, Gudmundsdottir AS, Sigurdardottir M, Chou TT, Nahmias J, Goss S, Sveinbjornsdottir S, Valdimarsson EM, Jakobsson F, Agnarsson U, Gudnason V, Thorgeirsson G, Fingerle J, Gurney M, Gudbjartsson D, Frigge ML, Kong A, Stefansson K, Gulcher JR. The gene encoding phosphodiesterase 4D confers risk of ischemic stroke. Nat Genet. 2003; 35: 131–138.CrossrefMedlineGoogle Scholar2 Helgadottir A, Manolescu A, Thorleifsson G, Gretarsdottir S, Jonsdottir H, Thorsteinsdottir U, Samani NJ, Gudmundsson G, Grant SF, Thorgeirsson G, Sveinbjornsdottir S, Valdimarsson EM, Matthiasson SE, Johannsson H, Gudmundsdottir O, Gurney ME, Sainz J, Thorhallsdottir M, Andresdottir M, Frigge ML, Topol EJ, Kong A, Gudnason V, Hakonarson H, Gulcher JR, Stefansson K. The gene encoding 5-lipoxygenase activating protein confers risk of myocardial infarction and stroke. Nat Genet. 2004; 36: 233–239.CrossrefMedlineGoogle Scholar3 Bevan S, Porteous L, Sitzer M, Markus HS. Phosphodiesterase 4D gene, ischemic stroke, and asymptomatic carotid atherosclerosis. Stroke. 2005; 36: 949–953.LinkGoogle Scholar4 Meschia JF, Brott TG, Brown RD Jr, Crook R, Worrall BB, Kissela B, Brown WM, Rich SS, Case LD, Evans EW, Hague S, Singleton A, Hardy J. Phosphodiesterase 4D and 5-lipoxygenase activating protein in ischemic stroke. Ann Neurol. 2005; 58: 351–361.CrossrefMedlineGoogle Scholar5 Lohmussaar E, Gschwendtner A, Mueller JC, Org T, Wichmann E, Hamann G, Meitinger T, Dichgans M. ALOX5AP gene and the PDE4D gene in a central European population of stroke patients. Stroke. 2005; 36: 731–736.LinkGoogle Scholar6 Nilsson-Ardnor S, Wiklund PG, Lindgren P, Nilsson AK, Janunger T, Escher SA, Hallbeck B, Stegmayr B, Asplund K, Holmberg D. Linkage of ischemic stroke to the PDE4D region on 5q in a Swedish population. Stroke. 2005; 36: 1666–1671.LinkGoogle Scholar7 O'Leary DH, Polak JF, Kronmal RA, Manolio TA, Burke GL, Wolfson SK Jr. Carotid artery intima and media thickness as a risk factor for myocardial infarction and stroke in older adults. Cardiovascular Health Study Collaborative Research Group. N Eng J Med. 1999; 340: 14–22.CrossrefMedlineGoogle Scholar8 Helgadottir A, Gretarsdottir S, St Clair D, Manolescu A, Cheung J, Thorleifsson G, Pasdar A, Grant SF, Whalley LJ, Hakonarson H, Thorsteinsdottir U, Kong A, Gulcher J, Stefansson K, MacLeod MJ. Association between the gene encoding 5-lipoxygenase-activating protein and stroke replicated in a Scottish population. Am J Hum Genet. 2005; 76: 505–509.CrossrefMedlineGoogle Scholar9 Dichgans M, Markus HS. Genetic association studies in stroke: methodological issues and proposed standard criteria. Stroke. 2005; 36: 2027–2031.LinkGoogle Scholar10 The International HapMap Consortium. A haplotype map of the human genome. Nature. 2005; 437: 1299–1320.CrossrefMedlineGoogle Scholar11 Humphries SE, Morgan L. Genetic risk factors for stroke and carotid atherosclerosis: insights into pathophysiology from candidate gene approaches. Lancet Neurol. 2004; 3: 227–235.CrossrefMedlineGoogle Scholar12 Jerrard-Dunne P, Sitzer M, Risley P, Buehler A, von Kegler S, Markus HS. Inflammatory gene load is associated with enhanced inflammation and early carotid atherosclerosis in smokers. Stroke. 2004; 35: 2438–2443.LinkGoogle Scholar13 Sebastiani P, Ramoni MF, Nolan V, Baldwin CT, Steinberg MH. Genetic dissection and prognostic modeling of overt stroke in sickle cell anemia. Nat Genet. 2005; 37: 435–440.CrossrefMedlineGoogle Scholar14 Lacombe P, Oligo C, Domenga V, Tournier-Lasserve E, Joutel A. Impaired cerebral vasoreactivity in a transgenic mouse model of cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy arteriopathy. Stroke. 2005; 36: 1053–1058.LinkGoogle Scholar15 Singhal S, Bevan S, Barrick T, Rich P, Markus HS. The influence of genetic and cardiovascular risk factors on the CADASIL phenotype. Brain. 2004; 127: 2031–2038.CrossrefMedlineGoogle Scholar16 Teasdale GM, Wardlaw JM, White PM, Murray G, Teasdale EM, Easton V, Davie Cooper; Scottish Aneurysm Study Group. The familial risk of subarachnoid haemorrhage. Brain. 2005; 128: 1677–1685.CrossrefMedlineGoogle Scholar17 Yamada S, Utsunomiya M, Inoue K, Nozaki K, Inoue S, Takenaka K, Hashimoto N, Koizumi A. Genome-wide scan for Japanese familial intracranial aneurysms: linkage to several chromosomal regions. Circulation. 2004; 14: 3727–3733.Google Scholar18 Nahed BV, Seker A, Guclu B, Ozturk AK, Finberg K, Hawkins AA, DiLuna ML, State M, Lifton RP, Gunel M. Mapping a Mendelian form of intracranial aneurysm to 1p34.3–p36.13. Am J Hum Genet. 2005; 76: 172–179.CrossrefMedlineGoogle Scholar19 Roos YB, Pals G, Struycken PM, Rinkel GJ, Limburg M, Pronk JC, van den Berg JS, Luijten JA, Pearson PL, Vermeulen M, Westerveld A. Genome-wide linkage in a large Dutch consanguineous family maps a locus for intracranial aneurysms to chromosome 2p13. Stroke. 2004; 35: 2276–2281.LinkGoogle Scholar20 Bergametti F, Denier C, Labauge P, Arnoult M, Boetto S, Clanet M, Coubes P, Echenne B, Ibrahim R, Irthum B, Jacquet G, Lonjon M, Moreau JJ, Neau JP, Parker F, Tremoulet M, Tournier-Lasserve E. Mutations within the programmed cell death 10 gene cause cerebral cavernous malformations. Am J Hum Genet. 2005; 76: 42–51.CrossrefMedlineGoogle Scholar Previous Back to top Next FiguresReferencesRelatedDetailsCited By Yamada Y (2020) Molecular basis of stroke Clinical Molecular Medicine, 10.1016/B978-0-12-809356-6.00012-5, (189-216), . Harrigan M and Deveikis J (2018) Ischemic Stroke Handbook of Cerebrovascular Disease and Neurointerventional Technique, 10.1007/978-3-319-66779-9_16, (827-918), . Avery M, Ogilvy C and Mitha A (2017) Cerebrovascular Disease☆ Reference Module in Neuroscience and Biobehavioral Psychology, 10.1016/B978-0-12-809324-5.02031-9, . Harrigan M, Deveikis J and Ardelt A (2013) Acute Ischaemic Stroke Agnieszka Anna Ardelt Handbook of Cerebrovascular Disease and Neurointerventional Technique, 10.1007/978-1-61779-946-4_17, (655-735), . Yamada Y (2012) Molecular Genetics of Stroke, Colloquium Series on Genomic and Molecular Medicine, 10.4199/C00052ED1V01Y201204GMM001, 1:1, (1-82), Online publication date: 31-Mar-2012. Hollingworth P and Williams J (2011) Genetic Risk Factors for Dementia The Handbook of Alzheimer's Disease and Other Dementias, 10.1002/9781444344110.ch6, (195-234), Online publication date: 13-Oct-2011. Wang G, Wang Y, Sun H, Cao W, Zhang J, Xiao H and Zhang J (2011) Variants of the arachidonate 5-lipoxygenase-activating protein (ALOX5AP) gene and risk of ischemic stroke in Han Chinese of eastern China, Journal of Biomedical Research, 10.1016/S1674-8301(11)60043-2, 25:5, (319-327), Online publication date: 1-Sep-2011. Chen K, Chang K, Chen H and Chen C (2011) Traditional Chinese medicine, a solution for reducing dual stroke risk factors at once?, Molecular BioSystems, 10.1039/c1mb05164d, 7:9, (2711), . Freitas R, Khaw K, Wu K, Bowman R, Jeffery H, Luben R, Wareham N and Rodwell S (2010) HMGCR gene polymorphism is associated with stroke risk in the EPIC-Norfolk study , European Journal of Cardiovascular Prevention & Rehabilitation, 10.1097/HJR.0b013e328330be77, 17:1, (89-93), Online publication date: 1-Feb-2010. (2009) Incidence of Stroke in Europe at the Beginning of the 21st Century, Stroke, 40:5, (1557-1563), Online publication date: 1-May-2009. Ogilvy C and Mitha A (2009) Cerebrovascular Disease Encyclopedia of Neuroscience, 10.1016/B978-008045046-9.00568-4, (801-806), . Ardelt A (2009) Acute Ischemic Stroke Handbook of Cerebrovascular Disease and Neurointerventional Technique, 10.1007/978-1-60327-125-7_17, (571-640), . Zhao H, Guan Q, Smith C and Quilley J (2008) Increased phosphodiesterase 3A/4B expression after angioplasty and the effect on VASP phosphorylation, European Journal of Pharmacology, 10.1016/j.ejphar.2008.05.016, 590:1-3, (29-35), Online publication date: 1-Aug-2008. Lin S, Hu C and Lin H (2008) Increased risk of stroke in patients who undergo cesarean section delivery: a nationwide population-based study, American Journal of Obstetrics and Gynecology, 10.1016/j.ajog.2007.10.789, 198:4, (391.e1-391.e7), Online publication date: 1-Apr-2008. Smeeton N, Heuschmann P, Rudd A, McEvoy A, Kitchen N, Sarker S and Wolfe C (2007) Incidence of Hemorrhagic Stroke in Black Caribbean, Black African, and White Populations, Stroke, 38:12, (3133-3138), Online publication date: 1-Dec-2007.Lee C and Kong M (2007) An Interactive Association of Common Sequence Variants in the Neuropeptide Y Gene With Susceptibility to Ischemic Stroke, Stroke, 38:10, (2663-2669), Online publication date: 1-Oct-2007. Avitsian R and Schubert A (2007) Anesthetic Considerations for Intraoperative Management of Cerebrovascular Disease in Neurovascular Surgical Procedures, Anesthesiology Clinics, 10.1016/j.anclin.2007.06.002, 25:3, (441-463), Online publication date: 1-Sep-2007. Koerner I, Jacks R, DeBarber A, Koop D, Mao P, Grant D and Alkayed N (2007) Polymorphisms in the Human Soluble Epoxide Hydrolase Gene EPHX2 Linked to Neuronal Survival after Ischemic Injury , The Journal of Neuroscience, 10.1523/JNEUROSCI.0056-07.2007, 27:17, (4642-4649), Online publication date: 25-Apr-2007. Patterson A, Pearl N and Chang C (2007) Impact of phosphodiesterase 4D on cardiac β2 adrenergic receptor signaling, Seminars in Anesthesia, Perioperative Medicine and Pain, 10.1053/j.sane.2006.11.002, 26:1, (22-27), Online publication date: 1-Mar-2007. , Clinical Chemistry and Laboratory Medicine, 10.1515/CCLM.2007.202, 45 Zhou X, Ji W, Tu Y, Yao M and Li Y (2007) Abdominal aortic aneurysm and cerebral aneurysm present different pathological evolutions and responses to pharmacological therapy, Medical Hypotheses, 10.1016/j.mehy.2006.06.062, 68:3, (601-606), Online publication date: 1-Jan-2007. (2007) BIBLIOGRAPHY The Biology of Human Longevity, 10.1016/B978-012373657-4/50008-8, (417-599), . van Leyen K, Kim H, Lee S, Jin G, Arai K and Lo E (2006) Baicalein and 12/15-Lipoxygenase in the Ischemic Brain, Stroke, 37:12, (3014-3018), Online publication date: 1-Dec-2006. Sauerbeck L (2006) Primary Stroke Prevention, AJN, American Journal of Nursing, 10.1097/00000446-200611000-00013, 106:11, (40-49), Online publication date: 1-Nov-2006. February 2006Vol 37, Issue 2 Advertisement Article InformationMetrics https://doi.org/10.1161/01.STR.0000200449.58684.8aPMID: 16410477 Manuscript receivedDecember 1, 2005Manuscript acceptedDecember 8, 2005Originally publishedJanuary 12, 2006 KeywordsstrokegeneticsCADASILPDF download Advertisement
Referência(s)