Fetal/neonatal alloimmune thrombocytopenia is a severe disease with devastating outcome in severely affected infants. Antenatal interventions suggest the most deleterious consequence, intracranial hemorrhage (ICH), is preventable without known risks for the mother and child. In these circumstances the most challenging issues include development of maternal testing to reliably predict fetal status and allow noninvasive antenatal strategies. Our study is the first to report information both on fetal platelet count and maternal alloantibody concentrations with 3 regimen therapies. Only HPA1b/1b women with a subsequent managed pregnancy after an index case leading to diagnosis, a complete obstetrical and sibling history, data on fetal and neonatal status, and analysis of maternal factors may be enrolled after informed consent. Therefore, among the cases referred to our laboratory, only 75 HPA 1b/1b women fulfilled these requirements (at-risk population) for a total of 239 pregnancies, 66 index cases, and 89 managed pregnancies (contrary to Sachs et al1 ).
Case reports may overestimate the clinical severity we observed. However the severity of clinical presentation and percentage of primigravida in newly diagnosed cases were very similar to previous larger cohort retrospective reports2-4
When biologic markers were analyzed careful consideration was given to (1) gestation range. The alloantibody concentration analysis was reviewed only with the first treated pregnancy of each mother (2) severity of the disease, platelet count < 50 × 109/L (3) timing of maternal samplings: at delivery means samplings done on delivery and NOT during the postnatal period. As reported elsewhere,5 we observed a noticeable increase in the postpartum concentration; therefore certain samples were excluded from analysis in the index cases (4) methodology used for alloantibody concentration6 (expressed as IU/mL as mentioned in “Methods” not observed by Sachs et al1 ).
These factors may explain apparent discrepancies between our results and other reports (retrospective versus prospective studies; among the anti–HPA-1a immunized mothers referred to our unit, 20% are not HLA DRB3*0101).
Cases were referred to our unit for therapy counseling; IVIG courses and steroids were therefore given without noticeable variations over the period of time and carefully controlled.
The goal of antenatal management is the prevention of severe fetal thrombocytopenia, with in utero ICH in 80% of cases. A safe fetal platelet count > 50 × 109/L may allow vaginal delivery. For ethical reasons no randomized controlled trials have been done for therapy against no treatment. Therefore, only observational studies are available. Reports, in some hundreds of cases,7 are in favor of maternal therapy with IVIG ± steroids. Giers et al8 report cases with repeated fetal blood samplings (FBS) before each IVIG course potentially playing a role in boosting the maternal immunization possibly explaining the poor results.
In this study without blind allocation the measure of the treatment effect was absence of ICH and the neonatal platelet count. To prevent ICH, the 3 therapeutic regimens were effective. Though each treatment had a failure rate, it is noticeable that combined therapy had the lowest percentage of neonates requiring postnatal therapy. The statistical analysis gave similar results even if siblings are not taken into account (only 51% of the index untreated cases were first newborns not as noted by Sachs et al1 ). This confirms that samples are independent.
At present the only available antenatal method to confirm response to therapy is FBS, which has a significant complication rate. Maternal alloantibody concentration threshold before therapy allows considering FBS for only 23.1% of the women, constituting considerable progress (NPV 76.9% and not 75% as noted by Sachs et al1 ). When followed during pregnancy over a greater number of cases (43 cases) it is still predictive of therapy failure (Table 1).
Follow-up of the maternal anti–HPA-1a antibody concentrations during managed pregnancies
| Weighted AUC, IU/mL . | Newborn platelet count, × 109/L . | P . | Se, % . | Sp, % . | PPV, % . | NPV, % . | |
|---|---|---|---|---|---|---|---|
| < 50 . | ≥ 50 . | ||||||
| < 24,n | 5 | 23 | |||||
| ≥ 24,n | 10 | 5 | .0049* | 66.7 | 82.1 | 66.7 | 82.1 |
| Weighted AUC, IU/mL . | Newborn platelet count, × 109/L . | P . | Se, % . | Sp, % . | PPV, % . | NPV, % . | |
|---|---|---|---|---|---|---|---|
| < 50 . | ≥ 50 . | ||||||
| < 24,n | 5 | 23 | |||||
| ≥ 24,n | 10 | 5 | .0049* | 66.7 | 82.1 | 66.7 | 82.1 |
n indicates number of newborns; Se, Sensitivity; Sp: Specificity; PPV, positive predictive value; and NPV, negative predictive value.
P < .05 (CI for α−risk of 5%)
In view of the rarity of this condition, collaborative studies are needed to accrue meaningful data and improve noninvasive strategies.
Authorship
Conflict-of-interest disclosure: The authors declare no competing financial interests.
Correspondence: Dr Cecile Kaplan, Platelet Immunology Unit, Institut National de la Transfusion Sanguine, 6 rue Alexandre Cabanel, Paris 75015, France; e-mail: ckaplan@ints.fr.
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