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Blood, Vol. 95 No. 11 (June 1), 2000:
pp. 3562-3567
RED CELLS
From the Department of Hematology/Oncology, Children's Hospital
Oakland, Oakland, CA; School of Public Health, University of
California, Berkeley, CA; Children's Hospital Oakland Research
Institute, Oakland, CA.
Cerebral infarction occurs in one quarter of all children with
sickle cell anemia (SCA). There is an increased risk of stroke in
siblings with SCA, suggesting genetic factors may influence risk of
stroke. The authors investigated whether HLA type was associated with
risk of stroke in children with SCA. Fifty-three patients with SCA
underwent complete HLA typing at both HLA class I (HLA-A, B) and HLA
class II (HLA-DR, DQ, DP) loci. Of the 53 patients, 22 had magnetic
resonance imagining (MRI)-documented evidence of cerebral infarction,
and the remaining 31 patients had negative MRI scans. Comparison of the
results of HLA typing between the SCA patients with a positive and
those with a negative MRI documented that the 2 groups differed with
respect to the class I HLA-B (P = .012), and the class II
HLA-DRB1 (P = .0008) and DQB1 (P = .029).
Susceptibility associations at the HLA-DRB1 locus included both DR3
alleles, where DRB1*0301 and *0302 were both associated with an
increased risk of stroke. Protective associations were found in the DR2
group, where DRB1*1501 was protective for stroke. DQB1*0201, which is
in linkage disequilibrium with DRB1*0301, was also associated with
stroke. Similarly, DQB1*0602, in linkage disequilibrium with DRB1*1501,
was protective. Specific HLA alleles may influence the risk of stroke
in children with SCA. HLA typing may prove useful in identifying SCA
patients at higher risk for stroke.
(Blood. 2000;95:3562-3567)
Stroke is one of the most devastating complications in
children with sickle cell anemia (SCA). Approximately 8% to 10% of children with SCA will suffer a symptomatic stroke, while 17% more
will have evidence of asymptomatic cerebral infarction with magnetic
resonance imaging (MRI).1-3 Even these latter, clinically occult lesions correlate with significant neuropsychological
deficits.4,5 The majority of strokes in children with SCA
(symptomatic or asymptomatic) are the result of infarction, with
intracranial hemorrhage becoming relatively more common later in
life.6 The most common location of infarction is in the
distribution of the anterior portion of the circle of
Willis.7,8 Arteriography or magnetic resonance angiography
often demonstrates progressive narrowing of these vessels with
collateral vessel development in a pattern similar to moyamoya
disease.9,10 Histopathologically, sickle cell vascular
lesions show a pattern of smooth muscle proliferation with overlying
endothelial damage.7,11 The abnormal adherence of sickle
red blood cells to the endothelium, as well as the altered rheology of
sickle red blood cells, undoubtedly contributes to the endothelial
injury in these vessels.12-15 Why every child with SCA does
not develop these histologic changes is unknown and suggests the
contribution of other environmental and genetic factors.
Anecdotally, it has been noted that stroke often occurs in siblings
with SCA,18-20 and an increased risk of stroke in siblings with SCA was recently suggested by a sib-pair study.17
Studies involving candidate genes known to influence coagulation have failed to show an association with cerebral infarction in
SCA.18-20 Because particular HLA types have been associated
with other vascular diseases characterized by endothelial
changes,21-25 we examined whether specific alleles in the
HLA region were associated with stroke in 53 children with SCA.
Study patients and design
MRI scanning
HLA typing Genomic DNA was extracted from 100 µL whole blood by means of the QIAGEN QIAamp 96 Spin Kit. DNA samples were typed at the HLA class II loci (DRB1, DQB1, and DPB1) with the use of the polymerase chain reaction, to amplify a locus-specific second-exon product, and analyzed with the use of sequence-specific oligonucleotide probes in a dot blot format as previously described.32,33 Class II haplotypes (DRB1-DQB1-DPB1) were inferred from linkage disequilibrium patterns.26,30,31 Samples were typed for HLA Class I A and B loci at an allelic level with the use of immobilized probe methods as previously described32,33 with modifications (personal communications, Drs R. Apple, T. Bugawan, and H. Erlich, Roche Molecular Systems, Alameda, CA). Class I typing methodology modifications from published methods included amplifying exons 2 and 3 separately in a multiplex reaction, and hybridization to modified and additional probes for exons 2 and 3 on our more optimized immobilized probe strips. For allelic level resolution, some sample types required subsequent dot blot probe hybridization using horseradish peroxidase-labeled exon 2 or 3 probes, and/or group-specific amplifications followed by immobilized probe analysis to distinguish them. Computer software programs were used to identify allelic types from the probe hybridization patterns. HLA alleles were classified according to nomenclature defined by the World Health Organization.34Statistical analysis Differences in HLA allele distributions between SCA patients with and without MRI-documented evidence of cerebral infarction were examined by means of row-by-column testing for independence using the log likelihood ratio or G test.35 This approach assumes that both alleles are statistically independent but avoids the multiple testing problem inherent in examining antigen frequencies. To deal with the problem of small expected values in contingency table testing of the highly polymorphic HLA loci, a Monte Carlo procedure was applied. The Monte Carlo procedure was used to determine the validity of the 2 distribution in testing a given table
without unnecessary binning of rare alleles.36 For each
locus tested, 10 000 replicate tables, based on the observed marginal
sums of a table, were generated. Row sums were binned into the
"combined" class only if the individual row sum was less than 5 for either the case or the control group. When row sums were binned as
necessary to achieve at least 5 entries, then the G values for the
overall row-by-column test were close to limiting values of the
2 distribution at the 0.10, 0.05, 0.01, and
0.001 quintiles. This resampling procedure is likely to be conservative
because any disease effect contributed by a rare allele will be hidden
in the combined class. The magnitude of significant individual allele effects for a locus showing overall significance were measured with the
odds ratio based on Fisher's exact test, calculated with probabilities.
Brain MRI results In 31 of the SCA patients, brain MRI results revealed no evidence of infarction. Of the 22 SCA patients with a positive MRI, 17 (77%) had a history of a clinically overt stroke. Of these 17 patients, 14 (82%) had evidence of large-vessel disease on MRI scans. The remaining 3 had watershed lesions. Five of the 22 patients (23%) with a positive MRI had a clinically silent stroke. Of these 5 patients, 3 (60%) had evidence of large-vessel disease, and the remaining 2 had watershed lesions.HLA typing results All 53 SCA individuals were typed at high (allelic) resolution for the HLA loci A, B, DRB1, DQB1, and DPB1. Allele frequencies from published control data from African Americans for the HLA class II loci DRB1, DQB1, and DPB1 were compared with the entire sample of SCA patients in order to validate the HLA composition of the study population as a random sample of African Americans. G tests of independence between the SCA and an outside control group were nonsignificant for each of the 3 loci, suggesting that our sample of pediatric patients, preselected for hemoglobin S homozygosity, did not differ from African Americans generally at the HLA loci.
HLA associations with autoimmune and infectious diseases have been
studied for more than 30 years and have provided insight into the
pathophysiology of many diseases.37,38 The HLA system serves as a master regulator of the immune system by directing the processing and presentation of foreign antigens to T
lymphocytes. While most diseases associated with HLA genes have a
recognized immune component, many do not. We present evidence that
particular HLA alleles are associated with the presence of cerebral
infarction in SCA. SCA is a well-characterized genetic disorder that
invariably results from the substitution of valine for glutamic acid at
the sixth position of the We are indebted to Henry Erlich for critical scientific review of
this manuscript.
Submitted August 26, 1999; accepted January 21, 2000.
Supported in part by National Institutes of Health grants HL-20985
and M01RR01271-16.
Reprints: Lori Styles, Department of Hematology/Oncology,
Children's Hospital Oakland, 747 52nd St, Oakland, CA 94609; e-mail:
lstyles{at}lanminds.com.
The publication costs of this
article were defrayed in part by
page charge payment. Therefore,
and solely to indicate this fact,
this article is hereby marked
"advertisement"
in accordance with 18 U.S.C.
section 1734.
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Top
Abstract
Introduction
globin molecule. The
clinical manifestations of this disease are heterogenous, and few
predictors for disease severity have been identified. The association
of HLA type with stroke provides the first evidence of a multi-genic
involvement in a specific manifestation of SCA. The idea that other
genes are likely to affect the clinical course of sickle cell patients is not new, but identification of genes and evidence of their involvement have been difficult. High fetal hemoglobin levels are known
to ameliorate the severity of sickle cell disease, and determination of
the factors that influence fetal hemoglobin expression has been
extensively studied. 
B transcription,
-thalassemia protect from early stroke in sickle cell anemia? [abstract].
Pediatr Res.
1986;10:285a.
an inflammatory disease.
N Engl J Med.
1999;340:115-126
