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The history of the Diego blood group

A história do sistema de grupos sangüíneos Diego

Abstracts

Diego blood group initially, because it appeared to be rare, was considered as a family or 'private factor'. With further investigation, it was possible to trace this blood group from an individual family in Venezuela to the Indians across the continent of America and eventually to the Mongolian race in Asia. This review article follows the developments over the years and the history of the Diego blood group.

Diego; blood group; history


O sistema de grupos sangüíneos Diego, devido à sua raridade, era considerado um fator privado familiar. Investigações posteriores, de estudos familiares na Venezuela e em índios do continente americano e mongóis na Ásia, evidenciaram a sua existência. Neste relato apresentamos o desenvolvimento do conhecimento e da sua história.

Diego; grupos sangüíneos; história


Artigo Especial

The history of the Diego blood group

Pedro C. Junqueira 1 1 - Honorary president of the Brazilian Society of Hematology and Hemotherapy, member of the Brazilian Academy of Medicine 2 - PhD, Researcher and Consultant in Immunohematology, Hemocentro, Unicamp

Lilian Castilho 2 1 - Honorary president of the Brazilian Society of Hematology and Hemotherapy, member of the Brazilian Academy of Medicine 2 - PhD, Researcher and Consultant in Immunohematology, Hemocentro, Unicamp

Diego blood group initially, because it appeared to be rare, was considered as a family or 'private factor'. With further investigation, it was possible to trace this blood group from an individual family in Venezuela to the Indians across the continent of America and eventually to the Mongolian race in Asia.

This review article follows the developments over the years and the history of the Diego blood group.

Keywords: Diego, blood group, history

Diego as a "Private Factor"

In 1953, Miguel Larysse and his co-workers Túlio Arends and R. Dominguez Sisco (from the Maternidad Concepcíon, Caracas) at the Centro de Investigaciones del Banco de Sangue de Caracas studied a serum from a full term male infant who appeared at birth to be clinically and hematologically normal but at that time the billirrubin determination was not carried out. Jaundice was evident after 12 hours, it became increasingly severe and the infant expired at three days. The direct antiglobulin test carried out on the newborn's red blood cells was positive. Blood specimens of the Rh-positive mother and her Rh-group compatible infant were sent to Philip Levine at his consultation service from Ortho Research Foundation (Raritan, New Jersey) and both samples arrived in excellent conditions in June. Although the infant's red cells were strongly "coated", no antibody was demonstrable in the maternal serum when it was tested with an extensive panel of selected cells, which, did not include the father's red blood cells. As ABO and Rh incompatibility was excluded, the occurrence of a "low-incidence" blood factor with its corresponding antibody was suspected.

On October 26th, 1953, the father of the dead infant visited Levine in New York. At this time his red blood cells were tested against the maternal serum and a strong agglutination reaction was found. Levine and the father agreed with the name of the blood factor as Diego (Dia).

Levine also demonstrated that Dia was not identical with two other previously recognized low-incidence blood factors associated with cases of hemolytic disease of the newborn named as Mia and Bea.

The Dia antibody was described as one of the six antibodies named as "Private" or "Family Blood Factors" (1). In this paper, they also reported that this antibody was "currently under investigation" at the Ortho Research Foundation and that it caused hemolytic disease and had negative reactions with 200 random white red blood cells tested. Table 1 shows the typing of red cell antigens in selected members of the Diego family.

Diego as an "Indian Factor"

In 1955, the mother of the first documented Dia antibody carrier consulted Layrisse about a new pregnancy, which permitted further and more extensive tests in Venezuela and at Raritan, New Jersey. Layrisse and collaborators studying four generations of the original Diego family, noticed that the third and fourth generations seemed to be Caucasoid but their skins were a little dark-brown. However, the members of the second generation and the great grandmother in the first generation had a dark-brown skin and they seemed to be of Mongolian origin. Taking into account this observation, they started to observe the physical characteristics of a population from different countries with 286 individuals who had been tested with an anti-Dia serum by the indirect antiglobulin test. The frequencies of positive results found in these populations were:

From these findings Layrisse et al., 1955 (2), concluded that it was evident that the Diego Factor was not restricted to a single family, and could be placed among the relatively high incidence blood group systems in Venezuela and probably in South America, with apparently genetic, anthropologic and clinical significances. They also commented that since the Diego terminology was meaningless and this factor had probably some anthropological implications it should be changed to a more expressive one like "Indian Factor". About this comment we must remember that Chown and Lewis (Nature, 1953) said that what appears to be a rare, private or family antigen in one population might be fairly frequent in another one, and so Layrisse was right.

In 1955, Dr Jean Dausset, a French immunologist, later awarded the Nobel Prize (1980), after working with Layrisse in Caracas, came to Rio de Janeiro to visit me because I was studying the Brazilians Indians. At the time, Dr Dausset brought me a sample of the Diego serum and this serum turned out to be very important to me. In that year we had the opportunity to test two Brazilian Indian groups with the anti-Diego serum using the indirect antiglobulin test: the Carajas living in Santa Izabel, Bananal Island, State of Mato Grosso and the Kaingaques living in a reservation near Palmas, State of Paraná. Thirteen (36%) of the red blood samples from the Carajas tested and 22 (46%) of the Kaingaques samples tested gave positive reactions with the anti-Diego serum. We had also the opportunity to test 200 red blood samples from true Black donors from the Rio de Janeiro Municipal Blood Bank that showed negative results with the anti-Diego serum. We sent our results to Layrisse, in Caracas and to Levine, in Raritan. We had our paper published in Nature, volume 17 on page 41 (3). Levine et al. published their paper in this same volume of the Nature Journal on page 40 (4).

Table 2 shows the incidence of the Dia antigen in different Indian populations.

Diego as a "Mongolian Factor"

In 1956, in a paper published in the Nature Journal (5), Layrisse and Arends stated: "Since the Indians of the American continent are considered to be anthropological related to the Mongolian people of the old world, we decided to investigate the incidence of the Diego Factor in other available representative Asians living in Venezuela". They tested 100 unrelated males from Canton (China), living in Venezuela, and detected 5 Diego positive individuals (5% of the Chinese tested). They also tested sixty-five unrelated Japanese and found 8 Diego positive subjects (12.5% of the Japanese tested) (6). These findings indicated that the Diego factor was not restricted to South America and suggested that this antigen was a Mongolian rather than an Indian factor.

In the same year, Lewis et al., (7) showed that the Diego antigen was found to be present in 16 of 148 unrelated Chippewa Indians from North Minnesota and in 6 of 77 unrelated Japanese from Winnipeg. This finding suggested that Diego might be an Asiatic characteristic.

In 1957, Levine and Robinson (8) said that studies carried out by Layrisse and his colleagues on the Diego blood factor in other populations including the Brazilian Indians carried out by Junqueira et al. (3), apparently suspected that the Diego factor could be Mongolian in its origin. Further, they concluded that the term Indian for the Diego blood factor was not appropriate.

Levine and Robinson, 1957 (8) also demonstrated that the Dia antigen was genetically independent from other 15 low incidence factors and from four high incidence factors previously recognized. Furthermore, Layrisse, Sanger and Race, 1959 (9) using evidence from the literature and from nine new families studied, showed that the Dia antigen had no links with most of the established blood group systems.

Many papers showing the distribution of the Dia antigen considered that it was essentially a Mongolian characteristic, absent in Whites , Blacks, Australian aborigines and other populations (10-39). Table 3 shows the incidence of the Dia antigen in the Chinese and Korean populations.

The book named "The distribution of Human Blood Groups and other polymorphisms" (Mourant et al., 1976) (40) is considered the best one to show the early worldwide race distribution of Dia..

In 1967, thirteen years after the detection of the anti-Dia, Thompson, Childers and Hatcher identified the anti-Dib (41). As the phenotype Di(a–b–) has not been reported yet, we may assume that only two alleles (Dia and Dib) control the Diego blood group system.

Both antibodies, anti-Dia and anti-Dib are responsible for the hemolytic disease of the newborn and for hemolytic transfusion reactions (42). Due to the composition of our population, and supported by studies showing that 3.6% of the multi-transfused patients in Brazil have anti-Dia (43) the Brazilian red cell panels used for antibody screening ought to include a Di(a+).

In 1975, Race and Sanger (42) said in the last edition (6th) of their book: "The Venezuelan discovery of Dia will make an outstanding contribution to the anthropology of the Mongolian world".

The Diego blood group system

The Diego blood group system is a rapidly expanding system and today it consists of two pairs of antithetical antigens (Dia and Dib, and Wra and Wrb) and 17 low incidence antigens (44) (Table 4).

Spring et al., in 1992 (45) recognized an association between band 3 (anion exchange 1 - AE1), the most abundant integral protein of the red blood cell (RBC) membrane, and the Diego blood group system. They found by SDS-PAGE that Di(a+) red cells always have band 3 variant Memphis, although not all band 3 Memphis red cells are Di(a+). This observation led to the investigation of band 3 from red cells of known Diego blood group in order to ascertain whether the expression of the Dia antigen is linked to band 3 Memphis, and to define the molecular basis of this variant.

In 1993, the Diego blood group locus was assigned to chromosome 17 by Zelinski et al., (46) and in 1994, Bruce et al. (47) showed by H2DIDS (4,4' –diisothiocyanato-2,2' –dihydrostibene disulfonate) binding studies on samples of known Diego phenotypes that the expression of the Dia antigen is associated with an increased susceptibility of band 3 to labeling by H2DIDS. This provided evidence for a link between the expression of the Dia antigen and the presence of band 3 variant Memphis (45).

DNA sequence analysis (47) showed that the Dia/Dib polymorphism results from a point mutation at nucleotide 2561 (C>T) resulting in a single amino acid substitution in position 854, with a proline corresponding to the Dib antigen and leucine to the Dia antigen. Molecular analysis of band 3 from individuals with red cells expressing the Dia antigen showed the simultaneous occurrence of the mutations 2561T (854Leu) and 166G (56Glu) responsible for the Band 3 variant Memphis (47).

Carries of band 3-Memphis are asymptomatic and show no morphologic abnormalities of their erythrocytes (48).Studies to determine the frequencies of band 3-Memphis in some populations have been performed, proving that band 3-Memphis is not a rare polymorphism and that the gene frequency of band 3-Memphis varies among different populations, with a high frequency among Indians and the Japanese (48-51).

Bruce et al. (1995) also reported that the Wra /Wrb polymorphism results from a glutamic acid in position 658 of band 3 corresponding to Wrb and a lysine in the same position, corresponding to Wra (52).

Evidence suggests that the Wrb antigen is also associated with the glycophorin A (GPA) because Wrb antigenrequires both band 3 and GPA for it's expression in the red cell membrane (52-54).

The recognition that band 3 carries antigens of the Diego blood group system and the elucidation of the Dia/Dib and Wra/Wrb polymorphisms have led several investigators to elucidate the molecular basis of the other low incidence Diego antigens and to create a more accurate structural model of band 3 (55).

New studies with band 3 and Diego are being developing and new findings are emerging. We have found in our population by molecular studies a high frequency of 166G mutations (Memphis) and the possibility that the Dia antigen can not be associated with the band 3 variant Memphis (56).

In the 1980s and 1990s, serological, biochemical and molecular studies have given a new face to Immuno-hematology. Most of the papers published are cooperative works and are improving the understanding of the Diego system. It is important that these studies should continue in different populations to expand the knowledge of the structure and function of band 3.

A história do sistema de grupos sangüíneos Diego

Resumo

O sistema de grupos sangüíneos Diego, devido à sua raridade, era considerado um fator privado familiar. Investigações posteriores, de estudos familiares na Venezuela e em índios do continente americano e mongóis na Ásia, evidenciaram a sua existência.

Neste relato apresentamos o desenvolvimento do conhecimento e da sua história.

Palavras-chave: Diego, grupos sangüíneos, história

Recebido: 28/06/01

Aceito: 13/02/02

Correspondência para: Pedro C. Junqueira

R. Prudêncio de Moraes, 985 - apto 104 - Rio de Janeiro - RJ - CEP: 22420-041 - fone: (21) 2522-9951

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  • 1
    - Honorary president of the Brazilian Society of Hematology and Hemotherapy, member of the Brazilian Academy of Medicine
    2
    - PhD, Researcher and Consultant in Immunohematology, Hemocentro, Unicamp
  • Publication Dates

    • Publication in this collection
      12 Aug 2002
    • Date of issue
      Mar 2002

    History

    • Accepted
      13 Feb 2002
    • Received
      28 June 2001
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