Reverse dot-blot detection of the African-American beta-thalassemia mutations

DNA-based diagnosis of the beta thalassemias provides accuracy to newborn screening genetic counseling, and prenatal diagnosis. However, the use of polymerase chain reaction (PCR)-based methods is challenged by the great number of different-beta-thalassemia mutations that exist even within defined ethnic groups. In this regard, the reverse dot-blot method offers a means of screening for several mutations with a single hybridization reaction. We have applied the reverse dot-blot method to the detection of the beta-thalassemia mutations of African-Americans. We used two biotin-labeled primer pairs in a duplex reaction to amplify and label two beta-globin target DNA fragments that encompass all known African-American beta-thalassemia mutations. The PCR products were denatured and hybridized to polyT-tailed, membrane-fixed, allele- specific probe pairs for the hemoglobin (Hb) S, Hb C, and 14 beta- thalassemia mutations and their corresponding wild-type sequences. Seven common mutations plus Hb S and Hb C were included on one diagnostic strip, and seven less common beta-thalassemia mutations were included on another strip. Carefully controlled, high stringency hybridization allowed accurate distinction of these alleles. Reverse dot-blot diagnosis of the less common beta-thalassemia mutations precludes the need for alternative, more technically challenging methods. This method provides a rapid, accurate method for diagnosis of beta thalassemia among African-Americans and other ethnic groups in which beta thalassemia occurs.

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The Relevance of the Social Control Theory in Explaining Crime among African American Families

Journal of Sociological Research ◽

10.5296/jsr.v8i1.10729 ◽

2017 ◽

Vol 8 (1) ◽

pp. 1

Author(s):

Ayodeji Daramola ◽

Gbolahan S Osho

Keyword(s):

African American ◽

Criminal Justice ◽

African Americans ◽

Control Theory ◽

Social Control ◽

Ethnic Groups ◽

Justice System ◽

African American Families ◽

Social Control Theory ◽

The Church

Today, criminologists, especially, Black criminologists, are thoroughly perplexed by the same problem of disproportionate minority confinement (DMC) most especially of Blacks in both the juvenile and criminal justice systems. Are African Americans more criminally minded than other races or ethnic groups? Do African Americans actually commit more crimes than others? These are the questions that the different deviant theories have tried to answer. The concept of social bonding arose from social control theory, which suggests that attachment to family and school, commitment to conventional pathways of achievements and beliefs in the legitimacy of social order are primary and important elements of establishing a social bond (Hirschi, 1969). In expounding his social control theory, Hirschi listed the elements of the bond as attachment, commitment, involvement, and belief. Does it mean that African Americans commit more crimes than other racial and ethnic groups? Or are African Americans genetically wired to be criminogenic? Is the society or the environment to blame for the perceived higher rate of crime among African Americans? Or are the criminal justice system, the judicial system, and the juvenile justice system, all together racially biased against Blacks, especially, Black males? Even though Hirschi (1969) did not mention attachment to religious beliefs as part of social control, but for the African American families, the church could play a significant role in helping to cement the bond of adolescents to their families. Any study of the African American family is not complete without the church. According to Work (1900), in all social study of the Negro, the church must be considered, for it is one of the greatest factors in his social life.

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Alpha and beta-Thalassemia mutations in Hubei area of China

BMC Medical Genetics ◽

10.1186/s12881-019-0925-5 ◽

2020 ◽

Vol 21 (1) ◽

Cited By ~ 1

Author(s):

Yaowu Zhu ◽

Na Shen ◽

Xiong Wang ◽

Juan Xiao ◽

Yanjun Lu

Keyword(s):

Mean Corpuscular Volume ◽

Southern China ◽

Hubei Province ◽

Beta Thalassemia ◽

Corpuscular Volume ◽

Dot Blot ◽

Inherited Disorders ◽

Great Heterogeneity ◽

Reverse Dot Blot

Abstract Background Thalassemia is a group of inherited hemoglobic disorders resulting from defects in the synthesis of one or more of the hemoglobin chains, which is one of the most prevalent inherited disorders in southern China. Only few studies reported the molecular characterization of α- and β-Thalassemia in Hubei Province in the central of China. Methods A total of 4889 clinically suspected cases of thalassemia were analyzed by Gap-PCR, PCR-based reverse dot blot (RDB). Results 1706 (33.8%) subjects harbored thalassemia mutations, including 539 (11.0%) subjects with α-thalassemia, 1140 (23.3%) subjects with β-thalassemia mutations, and 25 (0.51%) subjects with both α- and β-thalassemia mutations. Seven genotypes of α-thalassemia mutations and 29 genotypes of β-thalassemia mutations were characterized. --SEA/αα (66.05%), −α3.7/αα (24.12%), and -α4.2/αα (3.71%) accounted for 93.88% of the α-thalassemia mutations. βIVS-II-654/βN, βCD41–42/βN, βCD17/βN, βCD27–28/βN, βCD71–72/βN, β − 28/βN, β − 29/βN, βCD43/βN, βE/βN, accounting for 96.40% of all β-thalassemia genotypes. Furthermore, mean corpuscular volume (MCV) and mean corpuscular Hb (MCH) were sensitive markers for both β-thalassemia and α-thalassemia with --SEA/αα, but not -α3.7/αα and -α4.2/αα. Conclusions: Our data indicated great heterogeneity and extensive spectrum of thalassemias in Hubei province of China.

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The Role of Race on Survival after Alternative Donor Hematopoietic Progenitor Cell Transplant for Pediatric Acute Leukemia: Provocative Single Center Data.

Blood ◽

10.1182/blood.v104.11.5323.5323 ◽

2004 ◽

Vol 104 (11) ◽

pp. 5323-5323

Author(s):

David A. Margolis ◽

Mary Eapen ◽

Jeanette Carreras ◽

Julie-An Talano ◽

Meghen Browning ◽

...

Keyword(s):

Risk Factors ◽

African American ◽

African Americans ◽

Acute Leukemia ◽

Children And Adolescents ◽

Ethnic Groups ◽

Hematopoietic Progenitor Cell ◽

Unrelated Donor ◽

Alternative Donor ◽

Related Donor

Abstract Allogeneic blood or bone marrow transplant (BMT) can be a curative treatment for many children and adolescents with acute leukemia. With advances in unrelated donor transplant, others and we have shown that unrelated donor BMT can have similar survival to matched sibling BMT. There are several reports describing outcomes after matched related donor transplantation among various ethnic groups. Thus far, there are no published studies comparing outcomes among ethnic groups after alternative donor transplantation. Anecdotally, however, there have been concerns regarding outcomes among racial and ethnic groups, especially African-Americans. In order to address this question, we utilized our institutional database to analyze survival among children and adolescents receiving an alternative donor BMT at Children’s Hospital of Wisconsin from 1988-present. We compared survival in Caucasians and African-Americans undergoing unrelated donor and mismatched related donor transplantation (including haploidentical donors). One hundred and twenty four Caucasians underwent matched and mismatched unrelated donor transplantation compared to 11 African Americans. The 2-year probabilities of overall survival were significantly better for Caucasians at 53% (95% CI 44–62) than for African Americans, 18% (95% CI 2–45), p=0.01. Fifty-four Caucasians and 9 African Americans received mismatched family donor transplantation. Corresponding probabilities of overall 2-year survival were 38% (95% CI 25–51) and 30% (95% CI 5–64), respectively. Interestingly, our data show no statistically significant difference in survival after mismatched related donor transplantation between the Caucasian and African-American cohorts. Our data should be interpreted cautiously as the number of African Americans transplanted at our institution is few. Additionally, our analysis is limited by our inability to adjust for disease status at transplantation, HLA disparity and other known risk factors that may impact survival. Nevertheless these observations from a single institution cannot be ignored and warrant further analysis in a larger cohort such that outcomes after transplantation may be adjusted appropriately for relevant risk factors. We believe that a national database/registry study will have the numbers necessary to answer the questions that need to be asked regarding outcomes with alternative donor transplantation in the African-American population. We also believe that as cell processing and supportive care technologies improve mismatched family member transplantation outcomes, these advances could have a significant impact in improving leukemia-free survival for African-American children and adolescents.

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Rapid and simultaneous typing of hemoglobin S, hemoglobin C, and seven Mediterranean beta-thalassemia mutations by covalent reverse dot-blot analysis: application to prenatal diagnosis in Sicily

Blood ◽

10.1182/blood.v81.1.239.239 ◽

1993 ◽

Vol 81 (1) ◽

pp. 239-242 ◽

Cited By ~ 117

Author(s):

A Maggio ◽

A Giambona ◽

SP Cai ◽

J Wall ◽

YW Kan ◽

...

Keyword(s):

Globin Gene ◽

Blot Hybridization ◽

Beta Thalassemia ◽

Dot Blot ◽

Hemoglobin C ◽

Mediterranean Regions ◽

Analysis Application ◽

Working Day ◽

Dot Blot Analysis ◽

Reverse Dot Blot

Abstract The molecular lesions causing beta-thalassemia in Sicily can be subdivided into two groups. One that occurs at a 71% frequency and consists of the beta 39, IVS 1,110 and IVS 1,6 mutations and the other group at a 20% frequency comprising the -87, beta s, IVS 1,1 and IVS 2,745 mutations. The identification of all these mutations by polymerase chain reaction (PCR) and conventional dot-blot hybridization has been time consuming and expensive. In this article, we describe the implementation of the reverse dot-blot (RDB) hybridization as a rapid nonradioactive method for the identification of the nine most frequent molecular lesions in the beta-globin gene (-87, beta s, beta c, IVS 1,1, IVS 1,6, IVS 1,110, beta 39, IVS 2,1, IVS 2,745) in Sicily. Sixty prenatal diagnoses were performed by this RDB assay, each of which was confirmed by dot-blot/ASO hybridization; thus demonstrating the accuracy of the RDB. The main advantage of this assay is the rapid typing of an individual's DNA for many mutations in a single working day. Because the mutations in this assay are representative for the Mediterranean region, this mutational panel can also be extended to the screening of beta-thalassemia from other Mediterranean regions.

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Ethnic Differences in Polymorphisms and Haplotypes within the UGT1A Gene Complex.

Blood ◽

10.1182/blood.v104.11.3777.3777 ◽

2004 ◽

Vol 104 (11) ◽

pp. 3777-3777

Author(s):

Jeeranut Sawattep ◽

Thad A. Howard ◽

Noppawan P. Morales ◽

Yupin Sanvaridna ◽

Pranee Fucharoen ◽

...

Keyword(s):

African American ◽

Linkage Disequilibrium ◽

African Americans ◽

Drug Metabolism ◽

Phenotypic Variability ◽

Critical Role ◽

Beta Thalassemia ◽

Restriction Enzyme Digestion ◽

Gene Complex ◽

Promoter Polymorphisms

Abstract The UDP-glycosyltransferase (UGT1A) gene complex plays a critical role in the hepatic metabolism of a variety of chemicals, toxins, and drugs including bilirubin and acetaminophen. At least 13 different exon 1 sequences confer different binding specificities, while common exons 2–5 provide glycosyltransferase function. Mutations and polymorphisms within the UGT1A complex may help explain the phenotypic variability observed in drug metabolism. The frequency of three known polymorphisms in this complex: the UGT1A1 (TA)n promoter polymorphism (UGT1A1*28), and the UGT1A6 T181A and R184S mutations (UGT1A6*2), were determined in a cohort of Thai patients with HbE/beta-thalassemia (n=260) and African-American patients with sickle cell anemia (n=163), compared to published results for Caucasian persons (n=100). The UGT1A1 (TA)n promoter polymorphisms were identified by size discrimination using an ABI310® genetic analyzer, while the UGT1A6 mutations were identified using PCR amplification of the flanking sequence followed by restriction enzyme digestion at the polymorphic sites. The frequency of the abnormal UGT1A1 (TA)7 allele was lowest among Thai patients (0.15) and highest for African-American patients (0.48); Caucasians had an intermediate allelic frequency (0.29). The abnormal UGT1A1 7/7 genotype that confers the phenotype of Gilbert Syndrome was present in only 1.1% of Thai patients but was identified in 13.5% of African-American patients. Additional variant UGT1A1 alleles with 5 or 8 (TA) repeats were identified only in African-Americans. The frequency of both the T181A and R184S mutations within the UGT1A6 coding sequence ranged from 0.21 to 0.34, but were lower among both Thai and African-American patients than published values for Caucasians. Because these three genetic polymorphisms are known to be in linkage disequilibrium, the haplotype frequencies for the wildtype sequence (6/+/+) and the mutant sequence (7/−/−) were next estimated. Among African-Americans, the frequency of the 6/+/+ haplotype was 0.44, while the frequency of the 7/−/− was 0.14, totalling only 0.58 of the patients. Thai patients had a frequency of 0.73 for the 6/+/+ sequence and 0.09 for the 7/−/− sequence for a total of 0.82. Published values for Caucasians include a frequency of 0.66 for the 6/+/+ sequence and 0.28 for the 7/−/− sequence, for a total of 0.94. These data indicate that the UGT1A gene complex among Thai and African-American patients with hematological diseases has considerable variability compared to Caucasians. African-Americans have the highest frequency of variant UGT1A1 promoter polymorphisms and the lowest linkage disequilibrium, consistent with the older evolutionary timeframe in this population. Although Thai patients have a relatively low frequency of the abnormal UGT1A1 promoter allele and UGT1A6 mutations, they too have evidence of evolutionary drift. Taken together, these data suggest that common polymorphisms within the UGT1A gene complex may have important effects on the phenotypic variability observed in drug metabolism. Allele and Haplotype Frequency of UGT1A Polymorphisms Polymorphism Thai African-American Caucasian UGT1A1 (TA)5 .00 .07 .00 UGT1A1 (TA)6 .85 .48 .71 UGT1A1 (TA)7 .15 .37 .29 UGT1A1 (TA)8 .00 .07 .00 UGT1A6 T181A .21 .21 .32 UGT1A6 R184S .22 .26 .34 6/+/+ haplotype .73 .44 .65 7/−/− haplotype .09 .14 .29

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African-American Multiple Myeloma Patients Exhibit Less Bone Disease Compared to Other Racial/Ethnic Groups

Blood ◽

10.1182/blood.v116.21.4994.4994 ◽

2010 ◽

Vol 116 (21) ◽

pp. 4994-4994

Author(s):

Eric W. Dean ◽

Elad Ziv

Keyword(s):

Multiple Myeloma ◽

African American ◽

African Americans ◽

Ethnic Groups ◽

Bone Disease ◽

Conflicts Of Interest ◽

Compression Fractures ◽

Lytic Lesions ◽

Significant Difference ◽

Racial Ethnic

Abstract Abstract 4994 Background: Bone destruction remains one of the major complications in Multiple Myeloma (MM) leading to morbidity and mortality. African-Americans have a higher incidence of MM but exhibit longer survivals compared to Caucasians. We analyzed bone involvement in a cohort of patients with MM to determine if non African American (non AA) vs. African American (AA) race predicts the presence and severity of bone disease at presentation. Methods: Clinical data was gathered on 197 (176 non AA and 21 AA) MM patients at the University of California, San Francisco. Each patient had a skeletal survey at diagnosis and identified as having 0 lytic lesions, 1–2 lytic lesions or 3 or more lytic lesions. The presence of compression fractures was also documented for each patient as was age and sex. Results: The presence of compression fractures strongly correlated with the number of lytic lesions in both the non AA and AA groups, with no compression fractures observed in the patients with zero lytic lesions (p<0.001). Among the AA group, there were fewer (6 of 15) patients with compression fractures compared with patients from the non AA group (92 of 161) (p=0.02). There was also a trend towards fewer lytic lesions among the AA group (p=0.053). No significant difference was observed between the extent of bone disease and age or sex between the two groups. Conclusions: Within this cohort of patients, there is a significantly lower rate of compression fractures among African-Americans. These data supports the idea that African-American patients present with less bone disease which confers a survival advantage compared to other racial/ethnic groups. Disclosures: No relevant conflicts of interest to declare.

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Ethnic Differences in Magnesium Intake in U.S. Older Adults: Findings from NHANES 2005–2016

Nutrients ◽

10.3390/nu10121901 ◽

2018 ◽

Vol 10 (12) ◽

pp. 1901 ◽

Cited By ~ 2

Author(s):

Sarah Jackson ◽

Lee Smith ◽

Igor Grabovac ◽

Sandra Haider ◽

Jacopo Demurtas ◽

...

Keyword(s):

Older Adults ◽

African American ◽

African Americans ◽

Ethnic Groups ◽

Later Life ◽

Targeted Interventions ◽

Magnesium Intake ◽

Health And Nutrition ◽

Dietary Magnesium ◽

Using Data

Magnesium plays a crucial role in hundreds of bodily processes relevant to aging, but consumption of dietary magnesium intake has been shown to be inadequate in a large proportion of older adults. Identifying groups at risk of low magnesium intake is important for informing targeted advice. Using data from the National Health and Nutrition Examination Survey (NHANES) 2005–2016, we examined the association between ethnicity (Caucasian/African American/Hispanic/other) and magnesium intake in a large representative sample of U.S. older adults (≥65 y, n = 5682, mean (SD) 72.9 (0.10) y). Analyses adjusted for total energy intake and a range of relevant covariates. Overall, 83.3% of participants were not meeting the recommended level of dietary magnesium intake, ranging from 78.1% of other ethnic groups to 90.6% of African Americans. In the fully adjusted model, magnesium intake was lower among African American older adults (−13.0 mg/d, 95% CI: −18.8 to −7.2), and higher among Hispanics (14.0 mg/d, 95% CI: 7.5 to 20.5) and those from other ethnic groups (17.2, 95% CI: 3.8 to 30.5) compared with Caucasian older adults. These results highlight the need for targeted interventions to increase magnesium intake in U.S. older adults, with a focus on African Americans, in order to reduce the burden of morbidity and ethnic inequalities in health in later life.

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Evaluation of a commercial kit for microchromatographic quantitation of hemoglobin A2 in the presence of hemoglobin S.

Clinical Chemistry ◽

10.1093/clinchem/27.7.1244 ◽

1981 ◽

Vol 27 (7) ◽

pp. 1244-1247 ◽

Cited By ~ 4

Author(s):

R M Baine ◽

H G Brown

Keyword(s):

Sickle Cell ◽

Sickle Cell Anemia ◽

Sickle Cell Trait ◽

Accurate Method ◽

Beta Thalassemia ◽

Coefficients Of Variation ◽

Hb S ◽

Slow Moving ◽

Commercial Kit ◽

Hemoglobin A2

Abstract Commercial microcolumns introduced in 1976 by Helena Laboratories ("Hb A2 Quik Column") and by Isolab, Inc. ("Quik-Sep") provide a rapid, simple, accurate method for quantitation of hemoglobin A2 (Hb A2). However, these kits cannot be used for the quantitation of Hb A2 in the presence of slow-moving variants such as Hb S. Recently, Isolab, Inc., produced a new kit ("Quik-Sep Improved Hb A2 Test") for quantitation of both Hb A2 and Hb S. We compared results obtained with the new Isolab kit to results obtained with the original Tris/HCl method for quantitation of Hb A2 and Hb S. Blood was drawn from persons with sickle cell trait (A/S), sickle cell anemia (S/S), sickle cell/beta+ thalassemia (S/beta+ thal) and sickle cell/beta 0 thalassemia (S/beta 0 thal) and percentages of Hb A2 and Hb S were determined by each method. We found no significant differences in Hb A2 percentages by the two methods, and the coefficients of variation were similar. Both methods showed only slight overlap of Hb A2 values from subjects with some form of beta thalassemia and those with A/S or S/S. However, the Tris/HCl method consistently gave values for Hb S that were higher and closer to those expected, suggesting that the Isolab kit does not accurately quantitate Hb S.

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RACIAL DIFFERENCES IN NON-COGNITIVE SYMPTOMS IN ALZHEIMER’S DISEASE AND CAREGIVER DEPRESSION

Innovation in Aging ◽

10.1093/geroni/igz038.3150 ◽

2019 ◽

Vol 3 (Supplement_1) ◽

pp. S857-S857

Author(s):

Weizhou Tang

Keyword(s):

Alzheimer’S Disease ◽

Alzheimer's Disease ◽

African American ◽

African Americans ◽

Ethnic Groups ◽

Racial Differences ◽

Neuropsychiatric Symptoms ◽

Cognitive Symptoms ◽

Significant Group ◽

Caregiver Depression

Abstract Behavioral and psychological symptoms (BPS) represent a heterogeneous group of non-cognitive symptoms occurring in persons with Alzheimer’s disease (PwAD), and they are often associated with negative outcomes for AD caregivers. Evidence indicates differences in caregivers’ mental health across race/ethnic groups. However, there is a lack of research that compares racial differences in BPS in PwAD. This study aims to compare racial differences in BPS in PwAD and caregiver depression. The study analyzed data collected from the South Carolina AD Registry in 2010. The survey used in the interview included measures of caregiver depression, caregiver burden, PwAD’s non-cognitive symptoms, caregiving competence, caregiver distress, and demographics. The final analysis focused on 635 African-American (n=313) and white (n=322) caregivers. Mann-Whitney U-tests, Chi-square tests, and multiple linear regression were conducted. Among all PwAD, higher percentage of whites than African Americans exhibited apathy/indifference (67.52% vs 52.44%, p=.0001), depression/dysphoria (61.54% vs 44.59%, p<.0001), and anxiety (45.08% vs 29.64%, p<.0001). In terms of both frequency and severity of BPS, whites had significantly higher BPS score (Mean=35.49, SD=24.75) than African Americans (Mean=28.13, SD=23.97; p<.0001). Mean comparisons indicated significant group differences in caregiver depressive symptoms between white caregivers (mean=11.89, SD=6.90) and African-American caregivers (mean=9.41, SD=5.77). However, there were no racial differences in the relationship between BPS in PwAD and caregiver depression. The findings of this study highlight the importance of developing more effective and targeted treatment options and therapies for neuropsychiatric symptoms and delivering cultural relevant education programs/interventions to ethnic groups.

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Comparison of Measures of Socioeconomic Status between Ethnic Groups

Psychological Reports ◽

10.2466/pr0.1995.77.2.699 ◽

1995 ◽

Vol 77 (2) ◽

pp. 699-702 ◽

Cited By ~ 15

Author(s):

Terilee Edwards-Hewitt ◽

James J. Gray

Keyword(s):

College Students ◽

Socioeconomic Status ◽

African American ◽

Social Class ◽

African Americans ◽

Ethnic Groups ◽

Standardized Tests ◽

Socioeconomic Class

It has been hypothesized that African Americans report lower scores than Caucasians on standardized tests of socioeconomic status. College students were asked to report their family's socioeconomic class. In addition, the Revised Hollings-head four-factor socioeconomic questionnaire was given. Both groups surveyed, African American and Caucasian, underestimated their social class, but there were no differences between the groups.

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