Molecular Immunohematology in Ethiopian Sub-Populations
| Status: | Recruiting |
|---|---|
| Conditions: | Hematology |
| Therapuetic Areas: | Hematology |
| Healthy: | No |
| Age Range: | 18 - 99 |
| Updated: | 3/24/2019 |
| Start Date: | January 10, 2011 |
| Contact: | Traci Paige |
| Email: | td141n@nih.gov |
| Phone: | (301) 451-8655 |
Alloimmunization to blood products in transfused patients is a recognized management
challenge in the clinical setting. In particular the ethnic and racial specificity of RBC
antigens and the limited availability of matched healthy volunteer blood donors have
intensified the dilemma. The presence of low prevalence clinically significant RBC antigens
among minorities account for the higher rate of alloimmunization observed in patients from
this group. This is partly due to the racial and ethnic differences between the blood donor
and recipient populations in the US.
The increasing number of new Ethiopian-American immigrants in the US presenting to the health
care system with blood transfusion requirements makes understanding the unique transfusion
needs of this minority population imperative. Although the majority of African Americans
claim origin to West Africa, Ethiopians, being from East Africa, represent a rapidly growing
population in the United States. Furthermore, identifying genetic similarities and
disparities to their West African counterparts will certainly have clinical implications in
terms of transfusion support and disease modifiers. This additional information would help in
understanding the natural history and transfusion requirements of certain debilitating
diseases, such as Sickle Cell Disease, which are known to occur more commonly in African
Americans. Identifying ethnically and racially similar individuals could assist in recruiting
healthy volunteer donors with similar RBC antigen profiles potentially supplementing the rare
donor pool.
Although extensive archeological and sporadic serologic RBC antigen studies have been
conducted in Ethiopia there are no population wide RBC antigen molecular studies. Our study
population is selected by altitude and migration history. Ethiopia being in close proximity
to Red Sea in the northeast, Indian Ocean in the southeast and the rest of Africa in the
south/west has diverse population.
The study is a population based analysis of genetic variation of blood group antigens in
three distinct and conserved Ethiopian sub-populations. Statistical analysis using Chi-square
tests will be performed for each blood group antigen to detect differences in the
distribution between the three sub-populations. The investigators will travel to Ethiopia to
collect blood samples which will be analyzed in DTM at NIH using the standard serologic
methods and currently available molecular genotyping systems. Samples will also be stored for
future high throughput sequencing analysis and other studies.
The study will be a systematic analysis of the distribution of blood group antigens in
Ethiopian sub-populations. Furthermore, new variants could be detected allowing insight in
correlations of particular genotypes and phenotypes.
challenge in the clinical setting. In particular the ethnic and racial specificity of RBC
antigens and the limited availability of matched healthy volunteer blood donors have
intensified the dilemma. The presence of low prevalence clinically significant RBC antigens
among minorities account for the higher rate of alloimmunization observed in patients from
this group. This is partly due to the racial and ethnic differences between the blood donor
and recipient populations in the US.
The increasing number of new Ethiopian-American immigrants in the US presenting to the health
care system with blood transfusion requirements makes understanding the unique transfusion
needs of this minority population imperative. Although the majority of African Americans
claim origin to West Africa, Ethiopians, being from East Africa, represent a rapidly growing
population in the United States. Furthermore, identifying genetic similarities and
disparities to their West African counterparts will certainly have clinical implications in
terms of transfusion support and disease modifiers. This additional information would help in
understanding the natural history and transfusion requirements of certain debilitating
diseases, such as Sickle Cell Disease, which are known to occur more commonly in African
Americans. Identifying ethnically and racially similar individuals could assist in recruiting
healthy volunteer donors with similar RBC antigen profiles potentially supplementing the rare
donor pool.
Although extensive archeological and sporadic serologic RBC antigen studies have been
conducted in Ethiopia there are no population wide RBC antigen molecular studies. Our study
population is selected by altitude and migration history. Ethiopia being in close proximity
to Red Sea in the northeast, Indian Ocean in the southeast and the rest of Africa in the
south/west has diverse population.
The study is a population based analysis of genetic variation of blood group antigens in
three distinct and conserved Ethiopian sub-populations. Statistical analysis using Chi-square
tests will be performed for each blood group antigen to detect differences in the
distribution between the three sub-populations. The investigators will travel to Ethiopia to
collect blood samples which will be analyzed in DTM at NIH using the standard serologic
methods and currently available molecular genotyping systems. Samples will also be stored for
future high throughput sequencing analysis and other studies.
The study will be a systematic analysis of the distribution of blood group antigens in
Ethiopian sub-populations. Furthermore, new variants could be detected allowing insight in
correlations of particular genotypes and phenotypes.
Alloimmunization to blood products in transfused patients is a recognized management
challenge in the clinical setting. In particular the ethnic and racial specificity of RBC
antigens and the limited availability of matched healthy volunteer blood donors have
intensified the dilemma. The presence of low prevalence clinically significant RBC antigens
among minorities account for the higher rate of alloimmunization observed in patients from
this group. This is partly due to the racial and ethnic differences between the blood donor
and recipient populations in the U.S.
The increasing number of new Ethiopian-American immigrants in the US presenting to the health
care system with blood transfusion requirements makes understanding the unique transfusion
needs of this minority population imperative. Although the majority of African Americans
claim origin to West Africa, Ethiopians, being from East Africa, represent a rapidly growing
population in the United States. Furthermore, identifying genetic similarities and
disparities to their West African counterparts will certainly have clinical implications in
terms of transfusion support and disease modifiers. This additional information would help in
understanding the natural history and transfusion requirements of certain debilitating
diseases, such as Sickle Cell Disease (SCD), which are known to occur more commonly in
African Americans. Identifying ethnically and racially similar individuals could assist in
recruiting healthy volunteer donors with similar RBC antigen profiles potentially
supplementing the rare donor pool.
Although extensive archeological and sporadic serologic RBC antigen studies have been
conducted in Ethiopia, there are no population wide RBC antigen molecular studies. Our study
population is selected by altitude and migration history. Ethiopia, being in close proximity
to the Red Sea in the northeast, Indian Ocean in the southeast and the rest of Africa in the
south/west has diverse population.
The study is a population based analysis of genetic variation of blood group antigens in
three distinct and conserved Ethiopian sub-populations. Statistical analysis using Chi-square
tests will be performed for each blood group antigen to detect differences in the
distribution between the three sub-populations. The The Lead Associate Investigator (LAI),
and, as appropriate, additional
Investigators, will travel to Ethiopia to collect blood samples, which will be analyzed in
the Department of Transfusion Medicine (DTM) at the National Institutes of Health (NIH) using
the standard serologic methods and currently available molecular genotyping systems. Samples
will also be stored for future high throughput sequencing analysis and other studies.
The study will be a systematic analysis of the distribution of blood group antigens in
Ethiopian sub-populations. Furthermore, new variants could be detected allowing insight into
the correlation of particular genotypes and phenotypes.
challenge in the clinical setting. In particular the ethnic and racial specificity of RBC
antigens and the limited availability of matched healthy volunteer blood donors have
intensified the dilemma. The presence of low prevalence clinically significant RBC antigens
among minorities account for the higher rate of alloimmunization observed in patients from
this group. This is partly due to the racial and ethnic differences between the blood donor
and recipient populations in the U.S.
The increasing number of new Ethiopian-American immigrants in the US presenting to the health
care system with blood transfusion requirements makes understanding the unique transfusion
needs of this minority population imperative. Although the majority of African Americans
claim origin to West Africa, Ethiopians, being from East Africa, represent a rapidly growing
population in the United States. Furthermore, identifying genetic similarities and
disparities to their West African counterparts will certainly have clinical implications in
terms of transfusion support and disease modifiers. This additional information would help in
understanding the natural history and transfusion requirements of certain debilitating
diseases, such as Sickle Cell Disease (SCD), which are known to occur more commonly in
African Americans. Identifying ethnically and racially similar individuals could assist in
recruiting healthy volunteer donors with similar RBC antigen profiles potentially
supplementing the rare donor pool.
Although extensive archeological and sporadic serologic RBC antigen studies have been
conducted in Ethiopia, there are no population wide RBC antigen molecular studies. Our study
population is selected by altitude and migration history. Ethiopia, being in close proximity
to the Red Sea in the northeast, Indian Ocean in the southeast and the rest of Africa in the
south/west has diverse population.
The study is a population based analysis of genetic variation of blood group antigens in
three distinct and conserved Ethiopian sub-populations. Statistical analysis using Chi-square
tests will be performed for each blood group antigen to detect differences in the
distribution between the three sub-populations. The The Lead Associate Investigator (LAI),
and, as appropriate, additional
Investigators, will travel to Ethiopia to collect blood samples, which will be analyzed in
the Department of Transfusion Medicine (DTM) at the National Institutes of Health (NIH) using
the standard serologic methods and currently available molecular genotyping systems. Samples
will also be stored for future high throughput sequencing analysis and other studies.
The study will be a systematic analysis of the distribution of blood group antigens in
Ethiopian sub-populations. Furthermore, new variants could be detected allowing insight into
the correlation of particular genotypes and phenotypes.
- INCLUSION CRITERIA:
Individuals < 18 years of age will be excluded from the study. The study is a population
study and the information obtained from individuals above 18 years is not expected to be
different from those who are under 18 years old. Also, the need to involve adults to
consent individuals under 18 years old would be complicated. All donors should be healthy
volunteer individuals at the time of sample collection. Any potential donor with physical
and mental disability, individuals with known infectious and/or non-infectious diseases,
and pregnant women, are excluded from the study.
EXCLUSION CRITERIA:
Healthy Volunteers greater than or equal to 18 year of age. Volunteer healthy donors above
the age of 18 years, who have lived in the area since birth, and are at least 6 or 7
generation from endogenous families in the region, will be recruited. A detailed ancestral
line of descent (pedigree) is not mandatory to the study and will not be performed.
Individuals residing in rural regions are mostly conserved and it may be possible that some
donors could be closely related. However, to identify as diverse a population of potential
blood donors as possible, and avoid dilution of ancestral genes blood samples will be
collected from individuals known to reside in the region for generations and not known to
be closely related. Donors will be recruited through the local schools, churches, and
community organizations. The oral consent will include a question where each donor will be
asked if anyone in his/her family is also donating a sample, and, if so, how close the
relationship is to that individual. Blood collection will be on a firstcome, first serve
basis; individuals will be made aware that only one person among a group of close relatives
will be included in the study.
The study will be conducted in coordination with Addis Ababa University Medical Faculty and
the regional Health Offices in collaboration with Ethiopian Red Cross. The local PI, Dr.
Amha Gebgremedhin, is a member of the Addis Ababa University Medical faculty, Department of
Hematology, residing in Addis Ababa. The local health centers in the three regions listed
above will be used as centers for sample collection.
We found this trial at
1
site
9000 Rockville Pike
Bethesda, Maryland 20892
Bethesda, Maryland 20892
Phone: 301-496-4506
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