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View metadata, citation and similar papers at core.ac.uk brought to you by CORE Expert Reviews provided by Elsevier - Publisher Connector Obstetrics www.AJOG.org Pregnancy, parturition and preeclampsia in women of African ancestry AnnetteeNakimuli,MBChB,MMed(Obs&Gyn);OlympeChazara,PhD; JosaphatByamugisha,MBChB,MMed(Obs&Gyn),PhD;AlisonM.Elliott,MA,MBBS,MD,DTM&H,FRCP; PontianoKaleebu,MD,PhD;FlorenceMirembe,MBChB,MMed(Obs&Gyn),PhD; AshleyMoffett,MA,MB,BChir,MD,MRCP,MRCPath States are 4, 12, and 21, respectively, Maternal and associated neonatal mortality rates in sub-Saharan Africa remain unac- whereas those of Chad, Nigeria, and ceptablyhigh.InMulagoHospital(Kampala,Uganda),2majorcausesofmaternaldeath Congoare1100,630,and540per100,000 arepreeclampsiaandobstructedlaborandtheircomplications,conditionsoccurringat livebirths,respectively.InSSA,themajor the extremes of the birthweight spectrum, a situation encapsulated as the obstetric direct causes of maternal mortality are dilemma.Wehavequestionedwhethertheprevalenceofthesedisordersoccursmore hemorrhage, preeclampsia/eclampsia, frequentlyinindigenousAfricanwomenandthosewithAfricanancestryelsewhereinthe obstructed labor, and sepsis.4 Infections, worldbyreviewingavailableliterature.Weconcludethatthesewomenareatgreaterrisk pretermbirth,birthasphyxia,stillbirths, of preeclampsia than other racial groups. At least part of this susceptibility seems in- and small-for-gestational-age infants dependent of socioeconomic status and likely is due to biological or genetic factors. are the leading causes of perinatal Evidenceforageneticcontributiontopreeclampsiaisdiscussed.Wegoontopropose mortality.2,5 thattheobstetricdilemmainhumansisresponsibleforthissituationanddiscusshow Theseobservations are representative parturitionandbirthweightaresubjecttostabilizingselection.Otherdatawepresentalso ofourowninstitution,MulagoHospital suggest that there are particularly strong evolutionary selective pressures operating inKampala(Uganda)inwhichtheMMR duringpregnancyanddeliveryinAfricans.Thereismuchgreatergeneticdiversityand has remained high at 438 per 100,000 lesslinkagedisequilibriuminAfrica,andthegenesresponsibleforregulatingbirthweight live births, even though there has been andplacentationmaythereforebeeasiertodefinethaninnon-Africancohorts.Inclusion an increase in skilled birth attendance ofAfricanwomenintoresearchonpreeclampsiaisanessentialcomponentintackling (58%) and very good attendance rate thismajordisparityofmaternalhealth. (95%)atantenatalclinics.6 Key words: evolutionary selective pressure, great obstetric syndromes, length of Mulago Hospital is the busiest ma- gestation,obstetricdilemma ternityhospitalinSSA, servingasater- tiary referral center for Uganda. Details of deliveries and maternal deaths are shown in Table 1. Even with the lack Morethan90%ofmaternaldeaths partners, and others.1-3 The majority of of good medical records that is charac- worldwide occur in sub-Saharan these deaths are related to pregnancy teristic of much of SSA, our experience Africa(SSA)andsouthAsia.Thesehigh complications that are inadequately in Mulago Hospital is that causes of maternal and associated neonatal mor- managed because of a lack of access to maternal deaths are similar to the rest tality rates persist despite considerable emergency health care. The maternal ofSSA,withhemorrhage,preeclampsia/ efforts from the World Health Organi- mortality ratios (MMRs) of Sweden, eclampsia, and sepsis occurring very zation, governments, development the United Kingdom, and the United commonly.4,7,8 The large number of FromtheDepartmentofObstetricsandGynaecology,MakerereUniversityandMulagoHospital,Kampala,Uganda(DrNakimuliandDrsByamugishaand Mirembe);DepartmentofPathologyandCentreforTrophoblastResearch,UniversityofCambridge,Cambridge,UnitedKingdom(DrsChazaraand Moffett);MedicalResearchCouncil/UgandaVirusResearchInstituteUgandaResearchUnitonAIDS,Entebbe,Uganda(DrsElliottandKaleebu);and LondonSchoolofHygieneandTropicalMedicine,London,UnitedKingdom(DrElliott). ReceivedSept.11,2013;revisedOct.22,2013;acceptedOct.28,2013. ThisstudywassupportedbytheWellcomeTrust(grants090108/Z/09/Zand085992/Z/08/Zandavacationscholarshipin2011);theBritishHeart Foundation(grantPG/09/077/27964);theCentreforTrophoblastResearchattheUniversityofCambridge;andaWellcomeTrustUgandaPhD FellowshipinInfectionandImmunityheldbyA.N.,supportedbyaWellcomeTrustStrategicAward(grant084344). Theauthorsreportnoconflictofinterest. Reprints:AshleyMoffett,MA,MB,BChir,MD,MRCP,MRCPath,DepartmentofPathologyandCentreforTrophoblastResearch,Universityof Cambridge,TennisCourtRd.,CambridgeCB21QP,[email protected]. 0002-9378/$36.00 ª2014Mosby,Inc.Allrightsreserved. http://dx.doi.org/10.1016/j.ajog.2013.10.879 510 AmericanJournalofObstetrics&Gynecology JUNE2014 Expert Reviews www.AJOG.org Obstetrics women seen with preeclampsia, partic- ularly recurrent, severe, and early-onset TABLE1 DataforthematernityunitinMulagoHospital,Uganda preeclampsia and eclampsia, is of par- ticular concern to us because these Variable 2009 2010 2011 conditions have a high mortality and Livebirths 30,247 31,585 32,633 morbidity, are impossible to predict, Stillbirths 1260 1303 1230 andtheirpathogenesisisstillsomewhat mysterious. Cesareansections 6849 6702 6800 Here we review data relating to pre- Ruptureduterus 125 119 206 eclampsiainindigenousAfricansandin Maternaldeaths 187 152 188 women of African ancestry elsewhere Attendanceatantenatalclinic 78,157 76,673 69,129 intheworld.Wediscusstheideathatin these women, apart from the obvious, Nakimuli.Pregnancy,parturitionandpreeclampsiainAfrica.AmJObstetGynecol2014. cultural and socioeconomic factors and different priorities in health care, there areadditionalbiologicalreasonswhythe preeclampsia syndromes are such a prevalence of preeclampsia in SSA is PreeclampsiaamongAfrican prominentfeatureofAfricanobstetrics. unknown because detailed clinical re- Americans Our findings also lead us to question cords of all births are lacking. Dis- Although African Americans are obvi- whetherthereareothercharacteristicsof tinguishing between true preeclampsia ously not directly comparable with pregnancyandparturitionthatdiffer in and pregnancy-induced hypertension is indigenous Africans because of consid- Africanwomen. also difficult because proteinuria may erable genetic admixture (7-23%),18,19 not be adequately measured. A further the large number of reports and the Preeclampsiaandthegreatobstetric problem is a lack of information on consistencyofthefindingsareinforma- syndromes preexisting hypertension because pre- tive (Table 2). For decades it has been Animportantdeterminantofpreeclamp- sentationtotheclinicisoftenlate. clearthattherearedisparitiesinobstet- siaisfailureofplacentation,particularly Given this dearth of accurate records ric outcomes including preeclampsia thephysiologicaltransformationofspi- of pregnancy outcomes in Uganda and between AA and other groups; indeed, ral arteries, which leads to a stressed, SSA generally, to review the incidence black ethnicity is cited as a risk factor underperfused placenta.9,10 Preeclamp- of preeclampsia in women of African for preeclampsia in reviews.20,21 Of 4 sia is one of a spectrum of pregnancy ancestry, we have reviewed reports re- million births recorded in the National disorders that may result from this un- latingtopreeclampsiainAfricanAmer- Vital Statistics Report, pregnancy- derlying pathogenesis, including fetal icans(AA)and immigrantsfromAfrica associatedhypertensionwasmorecom- growth restriction (FGR), stillbirth, to other high-income countries as moninAA(5.0%)andleastfrequentin abruptio placentae, and some cases of compared with other ethnic groups. Hispanics(2.9%).22 preterm labor with intact membranes Studieswereidentifiedthroughasearch Astudyofmorethan2millionpreg- andprelaborruptureofmembranes.11,12 of the PubMed database for relevant nancies in New York using data from Because of the overlap in these condi- peer-reviewed articles published in En- hospital discharge records found that tions, it is useful to think of them to- glish using the search terms, pre- the rates of preeclampsia were substan- gether as the great obstetric syndromes eclampsia or eclampsia or hypertensive tially higher among AA compared with (GOS)(Appendix).13-15 disease in pregnancy or gestational hy- European Americans. This was even All these conditions are seen very pertensionorseverematernalmorbidity moreobviouswhenconfounderssuchas frequentlyinMulagoHospital.However, andethnicityorrace(Tables2and3). diabetes and maternal age were taken FGR cannot be reliably diagnosed In this review, we designate women into account. Furthermore, the differ- without accurate knowledge of gesta- of African ancestry as those women ence persisted after stratification for tional age, and low birthweight may descended from inhabitants of SSA. socioeconomic status based on area of resultfromavarietyofcauses.Similarly, Thereareobviouscaveatswhenreviewing residence.23 stillbirth is a heterogeneous condition datafromwomenofAfricandescentwho TwootherlargestudiesintheUnited thatcanresultfromcongenitalinfection, have migrated to new environments. States, each with more than 1 million birthasphyxia,orbirthtraumaaswellas Those who have the energy to migrate womenalsofoundthatpreeclampsiawas pooruteroplacentalperfusion. may be healthier than those left behind. more common in AA compared with Becausepreeclampsiaisarecognized Furthermore, factors such as diet, life- European Americans.24,25 One of these clinical entity characterized by new style,education,healthcare,climate,and studies took data from the National onset of hypertension and proteinuria indigenous pathogens are different and Inpatient Sample in which information after 20 weeks’ gestation, we have necessarily become an integral part of was also available on health insurance focusedonthisdisorder.16,17Theexact theimmigrant’snewenvironment. and income level; when this was taken JUNE2014 AmericanJournalofObstetrics&Gynecology 511 Expert Reviews Obstetrics www.AJOG.org TABLE2 PreeclampsiaoreclampsiastudiesamongAfricanAmericans Preeclampsiaor Cohortsize(total/AA) eclampsia,OR(95%CI) Comments Reference 2,571,069/450,098 1.67(1.64e1.71)a PEinwomeninNewYorkstate 23 1,030,350/161,780 1.59(1.49e1.69) Adjustedformaternalcharacteristicsandobstetrichistory 24 1,472,912/420,576 1.30(1.28e1.33) Adjustedformaternalcharacteristicsandobstetrichistory 25 299,499/n.a. 1.39(1.26e1.54)a SeverePEinwomenwithoutchronichypertension 26 206,428/19,512 2.12(1.85e2.42) Adjustedformaternalcharacteristicsandobstetrichistory 27 330/124 2.25(0.88e5.78) Eclampsia,adjustedformaternalcharacteristicsandobstetrichistory 29 4702/740 1.40(1.20e1.80) Adjustedformaternalcharacteristicsandobstetrichistory 30 271/38 2.50(0.97e6.40) Adjustedformaternalcharacteristicsandobstetrichistory 31 4314/1998 1.23(0.88e1.72) Adjustedformaternalcharacteristicsandobstetrichistory 32 153/35 2.27(1.26e5.92) LatepostpartumPE,notadjusted 33 2394/592 1.53(1.00e2.35) Adjustedformaternalcharacteristics,obstetrichistory,andbiochemicalfactors 34 103,860/13,748 1.36(1.27e1.45)a PEinwomenwithsingletonbirthatfirstdelivery 35 2,770,871/121,017 1.81(1.51e2.17) Eclampsia,adjustedformaternalcharacteristicsandobstetrichistory 36 127,544/12,639 1.41(1.25e1.62) Adjustedformaternalcharacteristics,chronichypertensionexcluded 28 16,300/6000 1.63(1.58e1.69)a Eclampsiainracialminorities,notadjusted,notsignificant 38 1355/374 3.20(1.04e9.93) PEinwomenwithoutchronichypertension 40 500/68 2.29(1.16e4.53) RecurrentPE,adjustedformaternalcharacteristicsandobstetrichistory 67 10,755/5555 1.30(1.07e1.58) Adjustedformaternalcharacteristics 44 2947/156 1.62(0.00e3.20) Noeffectwhenanalyzedbyrecruitmentcenter 69 Maternalcharacteristicsgenerallyincludematernalage,bodymassindex,andsmoking.Obstetrichistorygenerallyincludesparity,chronichypertension,anddiabetes. CI,confidenceinterval;n.a.,notavailable;OR,oddsratio;PE,preeclampsia. aORwascalculatedfromthedata. Nakimuli.Pregnancy,parturitionandpreeclampsiainAfrica.AmJObstetGynecol2014. into account, the findings remained the for both eclampsia and preeclampsia revealed a higher incidence of pre- same.24Theotherstudyuseddatafrom in nulliparous and parous women have eclampsia and eclampsia among AA womenwhowereallMedicaidenrollees also shown AA are at higher risk women compared with their European in14southernstates.25AAwomenwere (Table2).28-36 counterparts, irrespective of whether also most likely to have other poor Confounding factors such as obesity, therewaspreexistinghypertension.41 maternal outcomes like preterm labor, preexisting chronic hypertension, and Investigation of the GOS other than abruptioplacenta,andstillbirth. diabetes are difficult to control for and preeclampsia is more difficult because AnotherlargestudyfromtheNational are likely to contribute to the increased of the problems in accurate diagnosis Hospital Discharge Survey found AA risk of preeclampsia among AA, partic- described above. Nonetheless, a consis- women had a higher incidence of all ularly in the case of chronic hyperten- tent message is that ethnic disparities hypertensivedisordersinpregnancyand sion.37-39Thatpreeclampsiamaynotbe exist for all the GOS (spontaneous pre- a greater risk of severe complications of wholly explained by higher rates of term labor, FGR, stillbirth, and other preeclampsia such as abruptio placenta chronic hypertension among AAwomen poorobstetricoutcomes),andallhavean and stillbirth compared with European is suggested by a comparison between increased frequency among AA.26,42-45 Americans.26Similarfindingsweremade AfricanandEuropeanAmericanswithout In a study of more than 5 million inalargeWisconsinstudyrecruitedfrom chronic hypertension; the prevalence of births comparing birth outcomes be- hospitaldischargedata.AAwomenhad hypertension in pregnancy was similar, tween US-born and foreign-born thehighestriskforallthedifferenttypes but AA women still had an increased women, women of African ancestry of preeclampsia when compared with diagnosis of preeclampsia.40 Similar had the highest rates of infant mor- European American women.27 Several findingsweremademuchearlierbythe tality, low birthweight, and preterm other studies looking at risk factors Collaborative Perinatal project, which births, whether US born or foreign 512 AmericanJournalofObstetrics&Gynecology JUNE2014 Expert Reviews www.AJOG.org Obstetrics TABLE3 PreeclampsiastudiesamongrecentAfricanimmigrantstoothercountries Cohortsize Preeclampsia, (total/Africans) ORorRR(95%CI) Africanorigin Comments Location Reference 118,849/15,218 3.34(2.25e4.96) Caribbean Adjustedformaternalcharacteristics Canada 49 118,849/9130 3.14(2.04e4.83) SSA Adjustedformaternalcharacteristics Canada 49 2413/317 2.40(1.10e5.60) SSA,Surinam, Univariateanalysis TheNetherlands 50 Antilles 2506/29 2.70(1.20e6.20) Antilles EclampsiaincasesofSAMM,adjustedfor TheNetherlands 51 maternalcharacteristicsandobstetrichistory 2506/90 6.20(3.60e10.6) SSA EclampsiaincasesofSAMM,adjustedfor TheNetherlands 51 maternalcharacteristicsandobstetrichistory 6215/331 2.06(1.04e4.09) CapeVerde Adjustedformaternalcharacteristicsand TheNetherlands 52 obstetrichistory 6215/264 1.87(0.86e4.06) Antilles Adjustedformaternalcharacteristics TheNetherlands 52 andobstetrichistory 1728/576 2.47(1.02e6.00) Ethiopia Standardizedcarebetweenthegroups Israel 53 compared 76,158/11,395 2.60(2.32e2.92) Caribbean Adjustedformaternalcharacteristics UnitedKingdom 54 andobstetrichistory 8366/1581 3.64(1.84e7.21) n.a. Adjustedformaternalcharacteristics UnitedKingdom 55 andobstetrichistory 15,639/356 0.90(0.53e1.51)a SSA Noincreasedrisk Sweden 56 165,001/986 n.a. African,Somalia Noincreasedrisk Finland 58 526/158 3.90(1.70e8.94)a SSA Early-onsetPEcomparedtolateonset France 68 (<28or<34weeks) Maternalcharacteristicsgenerallyincludematernalage,bodymassindex,andsocioeconomicstatus.Obstetrichistorygenerallyincludesparity,chronichypertension,anddiabetes. CI,confidenceinterval;n.a.,notavailable;OR,oddsratio;PE,preeclampsia;RR,relativerisk;SAMM,severeacutematernalmorbidity. aORwascalculatedfromthedata. Nakimuli.Pregnancy,parturitionandpreeclampsiainAfrica.AmJObstetGynecol2014. born.46 In addition, the risk of pre- outcomes also apply to the Hispanic because these births often take place term birth, stillbirth, and low birth- population in the United States, yet incountrieswithgoodrecordsanduni- weight is increased not only in AA several studies have noted that pre- versalhealthcaresystems(Table3).For women but also with AA fathers.47,48 eclampsia, low birthweight, and still- example, a large study of more than Explanationsforthedisparitiesfound birth aresimilaroreven better than for 100,000 women who immigrated to between women with African or Euro- whitewomen,theHispanicparadox.28,44 Ontariobetween1985and2000showed peanancestryhavebeenpoorsocioeco- Using information from the Duke Uni- that the racial groups with the highest nomic status with lower incomes and versity Birth Database, AA women had risk of severe preeclampsia were from level of education, lack of medical in- higher rates of preeclampsia (10.2%) theCaribbeanorSSA.49 surance, poor utilization of precon- than the European (8%) or Hispanic Similar findings were made in The ception and antenatal services, stress, women (6.2%), even though the socio- Netherlands where the highest risk for discrimination, and residential segre- economic status of Hispanic and AA eclampsia and preeclampsia was from gation. Several reports have tried to womenwassimilar.44 womenfromSSA.50,51CapeVerdeanand determine the impact of these factors; Antilleanwomenwerealsoathigherrisk forexample,womenofAfricanancestry Preeclampsiaamongmorerecent ofpreeclampsiainareportfromRotter- were at an increased risk of pre- Africanimmigrantstoothercountries dam,TheNetherlands.52Alargenumber eclampsia in a second pregnancy, but LargenumbersofAfricanshavemigrated of Ethiopians have settled in Israel since this was not associated with Medicaid toEuropeandotherhigh-incomecoun- the 1980s where prenatal and obstetric enrollment.30 tries, mainly in the past 50 years. Ob- care is standardized with equal medical Many of the socioeconomic factors stetricoutcomesfortheserecentAfrican insurance, and in this group severe pre- that may contribute to poor obstetric immigrantsareinformative,particularly eclampsiawasmorelikelytooccur.53 JUNE2014 AmericanJournalofObstetrics&Gynecology 513 Expert Reviews Obstetrics www.AJOG.org Large groups of women of African Increased risk of other GOS, even if pregnancy,arealsoatincreasedrisk.73-77 ancestry live in London where access preeclampsia does not occur, is also Thesefindingsoffamilialaggregationin to National Health Service hospitals is clear from another large study in Swe- preeclampsia are also true for the other freely available and home deliveries are den, and other reports support this GOS.78-81 Although environmental fac- rare. In a survey of 80,000 pregnancies conclusion.35,63-66 tors, particularly influences acting in that included women of European and Largestudiesofthiskindarestillnot utero,areimportant,someoftheriskis Asian ancestry, 15% had African an- available for Africanwomen resident in likely to be genetic. Indeed, a study of cestry,andthiswasthesecondstrongest SSA,butourownexperienceinKampala female twin pairs with known zygosity riskfactorforpreeclampsiaafterchronic isthatrecurrentpreeclampsiadoesoccur estimated that the heritability of pre- hypertension and also carried a higher frequently. In London, 23% of 500 eclampsia was approximately 54%.82 risk of other poor obstetric outcomes womenwithpreviouspreeclampsiahad Could there be particular susceptibility such as FGR and stillbirth.54 Similarly, recurrent disease that required delivery genes associated with the higher fre- African ancestry was a risk factor for before37weeks, and African compared quency of preeclampsia in women of early-onsetpreeclampsiacomparedwith withEuropeanancestrywasasignificant Africanancestry?Acase-controlstudyof allotherracialgroups,andthisremained predictor.67 It also seems that when preeclampsia in Latinas, a group with so, even after adjusting for age, body preeclampsia does occur in the second admixturefromEuropean,African,and massindex,andothermaternalcharac- pregnancy in AA women, it is severe, native Americans, did show, using teristics.55 These and other studies of early-onset disease with associated FGR ancestryinformativemarkers,thatAfri- African immigrants also highlight the andpretermbirth.45Arecentstudyfrom can ancestry was associated with increasedriskofGOSsuchasstillbirths France suggests that women of African preeclampsia.83 andFGRsimilartoAA.56-58 ancestryaremoreatriskforearly-onset Theroleofthefetal(father’s)genesis preeclampsia and more likely to have lessobvious,butmanyreportsindicatea Severityandrecurrence had a previous history of preeclampsia paternal contribution to the risk.84-87 ofpreeclampsia compared with other groups, including Intergenerational and familial aggrega- The early onset and severity of pre- women from North Africa, despite the tionalsopointtogeneticfactorsderived eclampsiainwomenfromUgandaisalso evenhigherincidenceofchronichyper- frombothmaternalandfetalgenes,with a cause of concern, although the latter tensioninthelattergroup.68 most risk coming from maternal genes mayreflectthelateadmittancetoMulago thatmayactineitherthemotherorher Hospital. In a US national hospital Summary fetus.71,74,77,88 A drive to look for the discharge survey, higher mortality from Our comprehensive review of the liter- susceptibilitygenesforpreeclampsiahas preeclampsiaandeclampsiawasreported atureidentifiedveryfewpapersthatrun so far been disappointing. The studies among women of African ancestry countertoourconclusionthatwomenof generallyhavesmallnumbersofsubjects comparedwithEuropeanAmericans,but African ancestry are at increased risk of andhavenotbeenreplicated.89 only one-third or less of the difference developingpreeclampsia.First,3studies Genome-wideassociationscreening is couldactuallybeattributedtothehigher showed that these women were not at an unbiased approach to look for sus- prevalence.59 Pregnancy-related deaths increased riskof preeclampsia, but they ceptibilitygenesincomplexdisordersand from preeclampsia/eclampsia were 3 hadlowpowertodetectanyeffect.56,58,69 has been used in preeclamptic cohorts, times higher in AA women compared Second, the apparent increased suscep- but, although various single-nucleotide withEuropeans.60 tibility to preeclampsia among AA has polymorphism candidates have been In the UK Maternal Death Review beendismissedasaproblemofincorrect identified, the lackof statistical power is for the period 2006-2008, 22 deaths diagnosis.37 Third, race was discounted again a problem.90-93 Systematic meta- occurredasaresultofpreeclampsiaand as a significant risk factor for pre- analyses of these studies found 7 single- eclampsia. Despite being a minority eclampsia in another study, but data nucleotide polymorphisms significantly group, 6 of these deaths were Africans regarding AA women were combined associated near genes involved in pro- and the authors noted: “Black African withthatforotherminorityracessothat cesses such as coagulation, the renin- women seem particularly susceptible to the analysis could not provide a mean- angiotensinsystem,andinflammation. aggressive forms of preeclampsia. To ingfulcomparison.38 This highlights an important issue: establish if this is true, and what might searching for variants associated with be the underlying genetic or other Geneticsofpreeclampsia preeclampsia only in the maternal ge- pathophysiologicalmechanisms,further That there is a genetic component nomewillrevealgenesmainlyassociated researchisrequired.”61 to preeclampsia has long been sus- withthetertiarysystemicsyndromeand After a woman has had preeclampsia pected.70-72 Daughters of women with not those maternal and/or fetal genes inherfirstpregnancy,theriskofrecur- preeclampsia have more than twice the involvedinphysiologicaltransformation renceisincreased,witharelativeriskof risk of developing the disease them- ofthearteriesortothesubsequentstress 15.0citedinanauthoritativeNorwegian selves, and sisters of affected women, response of the placenta to the reduced study of more than 2 millionwomen.62 even if not born from a preeclamptic blood flow. The clear increased risk of 514 AmericanJournalofObstetrics&Gynecology JUNE2014 Expert Reviews www.AJOG.org Obstetrics cardiovascular disease in women who FIGURE1 havehadpreeclampsiaagainpointstoa MaternalKIR/fetalHLA-Cinteractionsatthesiteofplacentation separate set of susceptibility genes that are acting systemically and not during earlyplacentation.94,95 Wehavetakenadifferentapproachand focused on the primary defect of poor placentation. This is based on the idea that regulation of trophoblast behavior during placentation is mediated by allo- geneic recognition of trophoblast major histocompatibilitycomplexmoleculesby maternal lymphocytes.96 The findings that specialized immune cells, uterine natural killer (NK) cells, accumulate at thesiteofplacentation,togetherwiththe discovery of NKreceptors, the killer-cell immunoglobulin-like receptor family (KIR)andtheircognateHLA-Ctropho- blastligandshavedemonstratedhowthe mother can discern the presence of a geneticallydifferentindividual.97-99 KIR and HLA are the most poly- morphic gene families in humans, and we have shown that particular maternal KIR in combination with fetal HLA-C variantsareassociatedwithpreeclampsia and the other GOS.100-102 Women who have2KIRAhaplotypes(KIRAAgeno- type) are at risk when there is a HLA-C allele belonging to the C2 group in the fetus. Furthermore, the origin of the fetalHLA-C2isimportant;themostriskis fromaC2alleleinheritedfromthefather. We are now undertaking a similar study at Mulago Hospital, and pre- Inthese2 scenarios,the motherisHLA-C1 homozygousandthefetus hasinheritedan HLA-C2 liminary findings illustrate the same groupallelefromthefather.IfthemotherhasaKIRAAgenotypethatlacksactivatingKIRandhasa maternalKIR/fetalHLA-Ccombinations stronginhibitoryKIRforHLA-C2(KIR2DL1),poorplacentationresults.Incontrast,ifthemotherhasa associated with preeclampsia in African KIRABorBBgenotypecontainingtheactivatingKIRforHLA-C2(KIR2DS1),uterinenaturalkillercells women. Interestingly, the frequency of are triggered to produce increased amount of cytokines and chemokines (eg, granulocyte- the fetal HLA-C2 variant that confers macrophagecolonyestimulatingfactor)thatenhanceplacentation. riskisincreasedinUgandanscompared Nakimuli.Pregnancy,parturitionandpreeclampsiainAfrica.AmJObstetGynecol2014. with Europeans and Asians.103 Further- more, there is enormous variability of KIRgenesinAfricanswithfarmorege- women who have a protective KIR B receives sufficient nourishment for nor- notypes and more allelic variation at haplotype (in which the activating KIR maldevelopmentthroughremodelingof individualKIRloci.104 forHLA-C2,KIR2DS1,islocated)results thespiralarteries. How these genetic findings translate insecretionofcytokinesandchemokines intothefunctionofuterineNKcellsisa that may facilitate trophoblast invasion Theobstetricdilemma challenge,giventheethicalandlogistical andvasculartransformation.105Thus,we Overall, the data we have brought difficulties in experimenting with these proposethattheuterineimmunesystem together inthisreviewsuggestthatpre- cells.Functionally,wewouldpredictthat using highly variable maternal KIR/fetal eclampsia and other GOS occur more the risky combination results in very HLA-C interactions subtly defines the commonlyinwomenofAfricanancestry strong inhibition of uterine NK cells boundary between mother and baby, comparedwithotherethnicgroups,and (Figure1).TriggeringofuterineNKcells limitingthehighlyinvasiveplacentawhile thisisnotwhollyaccountedforbycon- by HLA-C2 target cells in vitro from at the same time ensuring the fetus founding social, cultural, and medical JUNE2014 AmericanJournalofObstetrics&Gynecology 515 Expert Reviews Obstetrics www.AJOG.org pelvic trauma, sepsis, and long-term FIGURE2 problems such as vesicovaginal fis- Birthweightandneonatalmortalityrates(n[13,730). tula.109 In Uganda, 2% of all women havehadanobstetricfistula.6Therefore, thehighercesareansectionratesseenin high-income countries in women of African ancestry may reflect not just delivery of women with preeclampsia but also an increased frequency of obstructedlabor.24,54,58,110 A detailed audit from the Royal Col- legeofObstetriciansandGynaecologists in the United Kingdom highlighted the higher cesarean section rates in women of African ancestry, even when con- founderssuchasage,parity,birthweight, and presentation were considered.110 Furthermore, shoulder dystocia has also been reported to occur more commonly inAAwomen.111 These findings may in part be accounted for by measurements of the bony pelvis revealing that there is even lessroomforthefetalheadinwomenof African ancestry. Although pelvimetry may not be a useful indicator in pre- dicting cephalopelvic disproportion in Adapted,withpermission,fromCavalli-SforzaandBodmer.108 individualpatients,112themeasurements Nakimuli.Pregnancy,parturitionandpreeclampsiainAfrica.AmJObstetGynecol2014. made of the pelvis, notably the pelvic inlet,outlet,lengthofsacrum,andpelvic influences.50,54,57,68Italsoseemsthatthe Compared with other primates, the floor area, are all smaller in women of risk of preeclampsia in African immi- passage of the large human fetal head Africanancestrycomparedwiththoseof grantstoEuropeisincreasedirrespective through a bony pelvis is a tight fit, Europeanancestry.113-115 of their area of origin in Africa, apart requiring rotationoftheheadasitgoes A possible consequence is that the from North Africans.68 All these obser- throughthebirthcanalasaconsequence fetal head engages into the pelvis late, vations point to a need to investigate of adaptation to bipedalism.106,107 The only when labor commences, whereas possible biological/genetic reasons con- high maternal and neonatal mortality thisoccursinthelastmonthofgestation tributing to the higher risk of pre- associatedwithextremesofbirthweight, in European and Asian women.116 eclampsiainSSA. sometimescalledtheobstetricdilemma, Several reports also document the fact Wewouldanticipatethattherewould has been described as “perhaps the thatnormalterminAfricanpregnancy be strong selective pressure against a most clear-cut example of a human occursatonlyapproximately38weeks’ disorderthat,withoutmedicalinterven- charactersubjecttostabilizingselection” gestation,whichis2weeksearlierthan tion, is frequently fatal to mother and (Figure2).108 in non-Africans, possibly facilitating child and occurs in 5-10% of firstpreg- Theoptimalsurvivalofbabiesweigh- birth before the baby becomes too nancies. A failure of the physiological ingbetween6and8lb(2.5-3.5kg)seems big.117-120Ifbirthsareoccurringearlier, transformation of uterine arteries is a tobeauniversalfeatureofhumanpop- itwouldcertainlythenbeadvantageous commonfeatureofalltheGOS,andthis ulations.Ifbabiesbecometoolarge,the for the fetus to mature more quickly, results in a reduced placental supply risk of obstructed labor is increased. As and indeed, African babies frequently of oxygen and nutrients, lower birth- intherestofSSA,atMulagoHospitalwe pass meconium with no sign of fetal weights, and the risk of preterm labor not only have many disordered preg- distress.119,121 There is also accelerated and superimposed preeclampsia. How- nancies arising from failure of placenta- lung maturity.122,123 Thus, the diffi- ever,atthesametime,wehavetoconsider tion, but we also experience frequent cultiesimposedbythebirthprocessand that maternal and neonatal mortality is births with prolonged obstructed labor the passage of the head and shoulders not only high under circumstances of because of cephalopelvic disproportion. through the bony pelvis seem to have reduced fetal nutrition but also when Without cesarean section, this leads to driven biological changes in many as- babiesaretoolargeforthepelvis. birthasphyxia,postpartumhemorrhage, pectsofpregnancy. 516 AmericanJournalofObstetrics&Gynecology JUNE2014 Expert Reviews www.AJOG.org Obstetrics Thiscleartrade-offbetweenthesizeof out-of-Africa migrations have reduced maternal death: a systematic review. Lancet the pelvis and head room will benefit theextentofgeneticvariationintheEu- 2006;367:1066-74. 5.LawnJE,CousensS,ZupanJ.Fourmillion babies who have intermediate birth- ropean populationsthat are thefocusof neonatal deaths: when? where? why? Lancet weights, and the 2 extremes with re- thegreatmajorityofstudiesofpregnancy 2005;365:891-900. duced survival will be selected against. disorders. 6.UgandaBureauofStatistics(UBOS)andICF Of interest will be a study of maternal Studyingbiologicaldiversitywillshed International Inc.Uganda Demographic and KIR/fetalHLA-Cvariantsinpregnancies light on pathological pregnancies in all Health Survey 2011, Kampala, Uganda. Kam- pala (Uganda): Ganda Bureau of Statistics withobstructedlaborastheKIRAandB populations, and inclusion of African (UBOS)andICFInternationalInc;2012. haplotypes and HLA-C1 and C2 groups women into research on preeclampsia 7.KayeD,MirembeF,AzigaF,NamulemaB. are under stabilizing selection and are is an essential component in tackling Maternalmortalityandassociatednear-misses foundatdifferentfrequenciesacrossthe thismajordisparityofmaternalhealth.It among emergency intrapartum obstetric re- world’spopulations.124 has been highlighted that “Africa is a ferrals in Mulago Hospital, Kampala, Uganda. Therefore,whenconsideringwhypre- geneticallyspecialplace”withgreaterge- EastAfrMedJ2003;80:144-9. 8.WandabwaJN,DoyleP,Longo-MbenzaB, eclampsia persists in populations, it is neticdiversityandlowerlevelsoflinkage et al. Human immunodeficiency virus and importantnotonlytoconsidertheGOS disequilibrium.126Thegenescontributing AIDS and other important predictors of but also the morbidity and mortality at to defective placentation are therefore maternal mortality in Mulago Hospital Com- the other end of the birth weight distri- likely to become obvious more quickly. plex Kampala Uganda. BMC Public Health 2011;11:565. bution. It may be that the consequences Indeed,ourinitialstudyofKIRgeneshas 9.Redman CWG, Sargent IL. Immunological of these contrasting selective pressures foundamuchgreaternumberofdifferent factors and placentation: implications for pre- notonlyaffecthigherbirthweightbabies KIR haplotypes in women delivering at eclampsia. In: Lyall F, Belfort M, eds. Pre- but also the tendency for enhanced MulagoHospitalbutalsohighlightedthe eclampsia. Cambridge (United Kingdom): numbersof undernourished babies with extentofvariabilityofthesegeneswithin CambridgeUniversityPress;2007. the concomitant maternal syndrome of the African continent.103 Denying the 10.RedmanCW,SargentIL.Latestadvances inunderstandingpreeclampsia.Science2005; preeclampsia.Thatistosaythatselection existenceofgeneticdifferencesinAfricans 308:1592-4. inapopulationforreducedfetalsizemay and their interactions with nongenetic 11.AnanthCV,VintzileosAM.Ischemicplacental lead to the persistence of factors predis- factorsonlydelaystheidentificationofthe disease: epidemiology and risk factors. Eur J posingtopreeclampsia. causalgenesorallelesthatwouldallowus ObstetGynecolReprodBiol2011;159:77-82. 12.Khong TY, De Wolf F, Robertson WB, to move away from racial/ethnic catego- Brosens I. Inadequate maternal vascular Futuredirections rization of individuals. Knowing the ge- response to placentation in pregnancies There is an urgent need to document netic variants will allow a better complicatedbypre-eclampsiaandbysmall-for- obstetric events better in SSA, and the understandingofthemolecularpathways gestational age infants. Br J Obstet Gynaecol lack of detailed electronic hospital re- and better health care for the women 1986;93:1049-59. 13.Brosens I, Pijnenborg R, Vercruysse L, cordsinthehospitalsaswellasthefail- carrying the risky genotypes, indepen- Romero R. The “Great Obstetrical Syndromes” uretorecordallbirthsinthepopulation dentlyfromtheirethnicity. - areassociatedwithdisordersofdeepplacenta- is a major difficulty for any maternal tion.AmJObstetGynecol2011;204:193-201. health research program. For example, ACKNOWLEDGMENTS 14.RomeroR,KusanovicJP,KimCJ.Placental proper assessment of gestational age at bed disorders in the genesis of the great Wethankalltheclinicalandresearchstaffofthe obstetricalsyndromes.In:BrosensI,Pijnenborg delivery will be crucial in the accurate Mulago Hospital and the patients and their R, Romero R, eds. Placental bed disorders: diagnosisoftheGOS.Therecordsystems familieswhomadethisworkpossible.Weare basic science and its translation to obstetrics. documenting obstetric and neonatal alsogratefultoGrahamBurton,HilaryCritchley, Cambridge, NY: Cambridge University Press; DavidDunne,andChristopherRedmanfortheir problemsarestillinadequatethroughout 2010:271-89. SSA,andthis is clearly a major priority. helpfulcommentsonthedraftmanuscript. 15.Smith GC. First-trimester determination of complications of late pregnancy. JAMA Introduction of record systems in 2010;303:561-2. 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AJOG.org. From the Department of Obstetrics and Gynaecology, Makerere Tennis Court Rd., Cambridge CB2 1QP, United Kingdom. [email protected]. of preeclampsia than other racial groups. At least .. because of cephalopelvic disproportion. Bjornsson H, Walker JJ, Snaedal G. Genetic and.
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