Sažetak | Uvod: Nasljedne razlike u ekspresiji RhD antigena na eritrocitnoj membrani nazivamo D
varijantama. Neke D varijante mogu razviti RhD imunizaciju, koja je vodeći uzrok hemolitičke
bolesti fetusa i novorođenčeta (HBFN). Različite D varijante na različit način reagiraju s
monoklonskim anti-D reagensima, što može dovesti do toga da D varijanta koja se može imunizirati
bude proglašena RhD pozitivnom.
Ciljevi: Ispitati pojavu RhD imunizacije kod trudnica s D varijantom te kliničke posljedice kod
njihove RhD pozitivne djece, odnosno pojavu HBFN. Analizirati D varijante koje su otkrivene u
rutinskom radu s korištenim monoklonskim anti-D reagensima, što podrazumijeva detaljnu serološku
analizu, RHD genotip te prevalenciju D varijanti među trudnicama Splitsko-dalmatinske županije.
Glavni cilj istraživanja je utvrditi je li moguće rutinskim serološkim testiranjem prepoznati nositelje
D varijanti koji su u riziku za RhD imunizaciju i tako spriječiti pojavu HBFN kod tih trudnica.
Metode: Provedena su dva neovisna istraživanja. Za Studiju 1 su retrospektivno prikupljeni podaci
o ukupnom broju trudnoća testiranih na RhD antigen, algoritmu ispitivanja RhD antigena, RhD
imunizacijama trudnica i njihovim kliničkim ishodima u dvadesetogodišnjem razdoblju.
U Studiji 2 su u devetogodišnjem razdoblju praćeni uzorci prvorotki koji nisu dali jaku pozitivnu
reakciju aglutinacije (4+) nego su označeni kao gradus 3+ ili manje, te su smatrani nejasnima i
podvrgnuti su proširenom serološkom ispitivanju RhD antigena u direktnoj i indirektnoj aglutinaciji,
a potom upućeni na genotipizaciju RHD antigena.
Rezultati: Studijom 1 su obuhvaćene 102,982 trudnoće. RhD imunizaciju razvile su 184 trudnice.
Od toga, tri trudnice su bile nositeljice parcijalnih D varijanti (jedna DNB, dvije DVa), što čini 1,63%
svih RhD imunizacija (CI 0,34;4,69), a sve tri su inicijalno bile određene kao RhD pozitivne. Ni u
jednom slučaju nije došlo do teške HBFN.
Studijom 2 je obuhvaćena 20,851 prvorotka. Devedeset šest trudnica (0,46%) je dalo slabe reakcije
aglutinacije u rutinskom serološkom ispitivanju. Od toga su RHD genotipizacijom 73 trudnice,
odnosno 0,35% (CI 0,27;0,44) određene kao slabi D, i to slabi D tip 1, slabi D tip 3 i jedan slučaj
slabog D tipa 29. Četrnaest trudnica, odnosno 0,06% (CI 0,03; 0,11) je određeno kao parcijalni D
kategorije DVa. Za dvije trudnice nije bilo moguće odrediti genotip varijante. Ostalih sedam trudnica
je proglašeno RHD pozitivnima. Prevalencija D varijanti otkrivenih serološkim metodama u našoj
populaciji prvorotki je 0,42% (95% CI 0,34;0;52), a najčešći parcijalni D antigen pripada kategoriji DVa. Sve nositeljice kategorije DVa su inicijalnim ispitivanjem bile ispravno prepoznate kao
vjerojatni parcijalni D antigen zahvaljujući jako pozitivnim reakcijama aglutinacije s klonom D7B8,
a slabim reaktivnostima (2+ ili manje) s klonom RUM-1.
Zaključak: RhD imunizacija se dogodila kod tri nositeljice parcijalnih D varijanti DVa i DNB. Ni u
jednom slučaju nije došlo do teške HBFN. Najznačajnija varijanta parcijalnog D antigena u našoj
populaciji je parcijalni D kategorije DVa. Monoklonski anti-D reagensi za ispitivanje trudnica i
primatelja transfuzije bi trebali biti odabrani tako da s DVa varijantom daju negativne ili slabe
reakcije kao što je stanična linija RUM-1, tako da tim osobama bude dodijeljen RhD negativan status. |
Sažetak (engleski) | Introduction: Hereditary differences in RhD antigen expression on red cell membrane are designated
as D variants. The carriers of some D variants are prone to RhD immunization. Anti-D is the leading
cause of hemolytic disease of fetus and newborn (HDFN). Different D variants give different
reactivities with monoclonal anti-D reagents. This can lead to immunization events, as they could be
mistakenly recognized as RhD positive.
Aims: To evaluate the occurrence of RhD immunization in pregnant carriers of D variants, as well
as the occurrence of HDFN in their RhD positive infants. To analyze D variants detected in routine
D typing using monoclonal anti-D reagents by performing extensive serologic analysis and RHD
genotyping. To determine the prevalence of D variants among pregnant women of Split-dalmatian
County.
The overall aim of the research is to determine if it is possible to successfully use routine serologic
methods for recognizing those D variant carriers that are in the risk of immunization, and by this to
prevent HDFN.
Methods: Two independent researches have been conducted. For Study 1, the data were
retrospectively collected on the number of pregnancies in which RhD antigen was determined, the
algorithm of RhD antigen typing, the RhD immunization events, HDFN occurrences and their
outcomes in pregnant women over a period of twenty years.
For Study 2, over a period of nine years we analyzed the samples of primiparous women which failed
to show strong reactions (4+) with anti-D reagents, but were graded 3+ or less instead. Their RhD
status was considered undetermined, and they underwent extensive serologic evaluation of RhD
antigen in direct and indirect agglutination, as well as RHD genotyping.
Results: Study 1 included 10.982 pregnancies. RhD immunization was detected in 184 pregnant
women, out of which three were partial D variant carriers (one DNB, two DVa variants), which
accounts for 1.63% of all RhD immunizations (CI 0.34;4.69). All three women were initially
designated RhD positive status. There were no cases of severe HDFN.
Study 2 included 20,851 primiparous women. Ninety-six of them (0.46%) gave weak agglutination
reactions in routine serologic typing. RHD genotyping showed 73 of them (0,35%; CI 0.27;0.44) to
be weak D types 1 or weak D type 3, with one case being weak D type 29. Fourteen women (0.06%;
CI 0.03;0.11) were genotyped as partial D variant DVa. Genotyping was unable to specify a D variant for two women. The remaining seven women were resolved as RHD positive. The prevalence of D
variants detected by serologic methods among primiparous women in our population is 0.42% (95%
CI 0.34;0.52). The most prevalent partial D variant is category DVa. All DVa carriers were correctly
recognized as probable partial D variants on their initial RhD typing, due to the strong positive
agglutination reactions with cell line D7B8 and weak reactions (score 2+ or less) with cell line RUM-
1.
Conclusion. RhD immunization occurred in three pregnant carriers of partial D antigen. There were
no cases of severe HDFN in their children. The most significant partial D variant in our population
is category DVa. Monoclonal anti-D reagents for testing pregnant women and transfusion recipients
should be chosen in a way that will ensure that they give negative or weak positive reactions with
DVa variant, such as cell line RUM-1. This will ensure that these individuals are assigned RhD
negative status. |