Background: ELI-P-Complex is the most advanced diagnostic test designed to assess whether the female body is ready (or unready) for the normal pregnancy course and for giving birth to a healthy child. ELI-P-Complex enables the perceived abnormalities to be individually treated even prior to the pregnancy planning, thus minimizing the risk of gestational and delivery-related complications. This prospective study shows the effectiveness of ELI-P-Complex testing during preconception care in women with a history of adverse pregnancy outcomes (APO). Methods: The data were reviewed from 4519 women with a history of APO and who planned to get pregnant. Following randomization, subjects of Group A were tested with ELI-P-Complex and treated before the pregnancy based on the results obtained. Group B subjects were not examined using the ELI- P-Complex test and were prepared for pregnancy in accordance with the standard strategy of pre- conception care [1]. Results: In Group A, gestational complications (GC) were revealed in 20% of women compared to 88.7% of Group B subjects; the relative risk (RR) of GC was 11.67 (95% CI: 9.9851 to 13.6392; P < 0.0001). APO was reported in 12% of Group A subjects vs. 38.1% of Group B ones; RR of APO was 5.8908 (95% CI: 4.9365 to 7.0296; P < 0.0001). Absolutely healthy children were born from 88.1% of Group A subjects compared to 50.3% of Group B ones; RR was 7.9601 (95% CI: 6.6110 to 9.5845; P < 0.0001). The positive predictive value, sensitivity, and specificity of the test for GC were 93.82% (95% CI: 92.72% to 94.80%), 93.17% (95% CI: 92.03% to 94.20%), and 92.62% (95% CI: 91.31% to 93.78%), respectively. Conclusions: The use of ELI-P-Complex for examination and further preconception care in women with a history of APO considerably reduces GC, improves pregnancy outcomes, and increases chances of giving birth to a healthy child.
Adverse pregnancy outcomes (APO), primarily including miscarriages, intrauterine fetal death, and giving birth to children with developmental malformations, are observed rather often. Miscarriage affects at least 10% of couples trying to conceive, while one in every 33 babies in the United States is born with a birth defect [
It is known that only a small part of APO (5% - 13%) is caused by genetic aberrations, while most birth defects and miscarriages are associated with epigenetic developmental disorders [
Recently a laboratory diagnostic test called ELI-P-Complex [
The study was conducted from April 2008 until June 2014 (the last participant was enrolled in March 2013). Initially, 4519 female patients aged 17 to 45 years were enrolled for its conduction; they visited special family planning centers in Moscow, Saint-Petersburg, Kazan, Novosibirsk, and Rostov-on-Don (Russian Federation). Later, all study participants were followed up in out-patient service at Obstetrics and Gynecology Departments in nineteen hospitals of the above-mentioned cities. For delivery, as well as in case of any pregnancy complications, all participants were mandatorily hospitalized in these particular hospitals.
The main criterion for inclusion in the study was the presence in the medical history at least one of the following adverse pregnancy outcomes: miscarriage, missed miscarriage, anembryonic pregnancy (blighted ovum), fetal death (stillbirth), intrauterine growth restriction, premature birth, and fetal and congenital malformations. Fertile women without a history of adverse pregnancy outcomes, as well as women diagnosed with infertility, were withdrawn from the study. The study was approved by the research ethics committees at all participating hospitals, and women gave informed consent before enrolling in the study.
Women who were eligible for the study were randomly allocated to two groups: the group of preconception care based on ELI-P-Complex testing data (Group A, n = 2209) and the group of preconception care without ELI-P-Complex testing (Group B, n = 2310) (
Blood serum samples were drawn from all women in Group A prior to the pregnancy for testing with ELI-P-Complex. Freshly obtained blood serum samples stored for not longer than 3 days at a temperature = +1˚C ∙∙∙ +4˚C were used in the study. Analysis was conducted using ELI-P-Complex kits (Immunculus, Moscow).
ELI-P-Complex method. ELI-P-Complex method and kit are intended for measuring the profiles of specific serum immune reactivity (IR) which depends on a serum content of twelve IgG a-Abs [
Median individual immune reactivity (MIR) and profiles of individual immune reactivity (relative content) of the corresponding auto-antibodies were detected and analyzed in the blood serum samples.
Reactions were run according to the manufacturer’s instructions using standard procedures of enzyme-linked immunosorbent assay. The optical density level of the immunosorbent reaction of the control serum (CS) with each antigen was considered as 100%, and the intensity of the patients’ serums reactions with the same antigens was calculated relative to the CS reaction [
Abbreviations: MIR―median individual level of immune reactivity of the individual patient’s serum regarding
Characteristic | Group A (n = 2209) | Group B (n = 2310) | P |
---|---|---|---|
Maternal age (years) ≥30 <30 | 1489 (67.4%) 720 (32.6%) | 1483 (64.2%) 827 (35.8%) | P < 0.05 P < 0.05 |
Gynecological diseases in the past medical history | 1953 (88.4%) | 2107 (91.2%) | Р < 0.05 |
Outcomes of previous pregnancies Full term birth Premature birth Fetal and congenital malformations Fetal death (stillbirth) Induced abortion Miscarriage 1 2 3 and more Missed miscarriage Anembryonic pregnancy (blighted ovum) Intrauterine growth restriction | 528 (23.9%) 60 (2.7%) 82 (3.7%) 53 (2.4%) 371 (16.8%) 581 (26.3%) 985 (44.6%) 596 (27%) 400 (18.1%) 75 (3.4%) 176 (8%) | 566 (24.5%) 51 (2.2%) 67 (2.9%) 62 (2.7%) 418 (18.1%) 621 (26.9%) 1088 (47.1%) 573 (24.8%) 411 (17.8%) 90 (3.9%) 166 (7.2%) | Р > 0.05 Р > 0.05 Р > 0.05 Р > 0.05 Р > 0.05 Р > 0.05 Р > 0.05 Р > 0.05 Р > 0.05 Р > 0.05 Р > 0.05 |
all the used antigens. The normal (physiological) levels of individual MIR are restricted by the ranges −30% ∙∙∙ to 0% (or conditional units (CU)) of the control sample median IR.
Moreover, in order to analyze immune reactivity profiles of the studied patients, a deviation (as a percentage of the individual median normalized reaction level) detected in the serum of a studied patient was calculated for each of the antigens using the following formulas:
Abbreviations: R(nrm)ag1, ag2, ∙∙∙, ag12―deviation (in fractions of the individual median normalized reaction level) detected in the individual patient’s serum for each of the used antigens −1, −2, ∙∙∙ −12; OD (ag1, ag2, ∙∙∙ ag12)―optic density of the individual patient’s serum reaction with each of the used antigens −1, −2, ∙∙∙ −12; OD(k1, k2 ∙∙∙ k12)―optic density of the CS with each of the used antigens −1, −2, ∙∙∙ −12. The normal (physiological) level of each a-Ab is restricted by the ranges −20% ∙∙∙ to 10% (or conditional units (CU) from the individual average IR). A special computer program supplied together with the kits was used for calculations.
In Group A, disorders revealed with ELI-P-Complex test were confirmed by routine methods of diagnostics according to the unified criteria for patient examination recommended after ELI-P-Complex testing. Treatment of detected disorders was conducted individually in accordance with the common methods of disease treatment. In 3 - 4 weeks after the treatment completion, a control examination was conducted using ELI-P-Complex test. In this study, absolutely all women were allowed to plan pregnancy regardless of the test result solely for scientific purposes; however, the manufacturer of ELI-P-Complex test recommends pregnancy planning strictly according to the following criteria: 1) normalization of the serum content of embryotropic a-Abs; 2) decrease in initially elevated level of the immune reactivity of certain a-Abs by at least 50% from baseline; 3) increase in median individual reactivity (MIR) level of at least 1.5 fold the initial value in women with immune suppression at baseline; and 4) decrease in the median individual reactivity (MIR) level to the normal values in women with initial immune activation. Absence of the above-mentioned changes indicates that the treatment is not effective and a specific pathogenic cause persists which can result in recurrence of the adverse pregnancy outcome.
Pregnancy onset in Group A was registered 3 - 9 months after the first investigation with ELI-P-Complex test. In total, pregnancy was diagnosed in 1971 women from Group A. In 238 cases pregnancy did not happen during the 6-month period of observation, and such patients were excluded from the study. In Group B, preconception care was not conducted using ELI-P-Complex test, and the women started pregnancy planning right after randomization. In Group B, pregnancy was confirmed in 1998 women. In the remaining 312 women, pregnancy did not occur within 6 months and they were withdrawn from the study.
In both groups (Group A and Group B), ELI-P-Complex test was performed during the first, second, and third trimester, as well as all standard laboratory tests, ultrasound scanning to assess the pregnancy course, the condition of mother and child, and also the condition of a newborn right after the delivery. Clinical monitoring of the pregnancy course was initiated at weeks 6 - 9 of gestation and was continued until its completion. Health state of children delivered by women under observation was assessed within the first 5 - 7 days after birth (
All statistical analyses were performed using the SPSS 21.0.0 for Windows (IBM, NY, USA) and STATA/SE 13.0 software (STATA Corp., Texas, USA) taking into consideration 95% CI. The chi-square test was used to determine significant differences. Performance indicators (positive predictive value (PPV), sensitivity, specificity) of ELI-P-Complex test have been calculated for pregnancy complications. Relative risk of an adverse pregnancy outcome and delivery of an unhealthy child was calculated by comparing Group A (with preconception care with ELI-P-Complex testing) and Group B (without ELI-P-Complex testing during the preconception care).
Initially almost 2209 non-pregnant women with a history of adverse pregnancy outcomes were tested using ELI-P-Complex (Group A). It was found that disorders of serum immune reactivity determined by natural IgG auto-antibodies are revealed in more than 90% of such women: abnormalities were reported in 92.4% (n = 2041) of them, and only in 7.6% (n = 168) of patients ELI-P-Complex test scores were within the normal range. The changes revealed included abnormal decrease or, vice versa, abnormal increase in total immune reactivity level in the blood serum with all or with the most of the used antigens (abnormalities of the median individual immune reactivity, MIR). Furthermore, abnormal changes could selectively relate to separate a-Abs of certain specificity.
Additional clarifying investigations prescribed based on screening ELI-P-Complex data made it possible to specify in detail the situation in each case. In 83.5% (n = 1704) of women from Group A, abnormal increases in microbial population potentially important for adverse pregnancy outcome (including chlamydia, mycoplasma, ureaplasma, gardnerella, trichomonasvaginalis, candida, and herpes viruses) was detected. In 65.6% (n=1339) of women, hormonal disorders of various grades were revealed (thyroid disorders, disorders of menstrual cycle, polycystic ovary syndrome, hyperandrogenism, hyperprolactinaemia, hypogonadism, hypoprogesteronaemia, and obesity). In 8.2% (n = 167) of cases, the signs of pancreatitis were revealed; notably, in almost a quarter of such women (n = 38) the signs of glucose intolerance and/or metabolic syndrome were observed. In some of the examined women, the signs of antiphospholipid syndrome (18.6%, n = 380) were present; small vessels vasculitis (12.1%, n = 245), thrombocytopathy (9.1%, n = 186), and changes in hemostasis (8.3%, n = 169) were revealed in nearly one third of patients. An abnormally elevated level of antibodies against chorionic gonadotropin was detected in 3.4% of women (n = 69), pituitary adenoma was revealed in 2 (0.1%), and the signs of premature ovarian aging were observed in 9 (0.44%) of women. The signs of papillomavirus infection were revealed quite often (in 24.4%, n = 498) which is a rather common cause of pathologic pregnancy. Rather often (16.8%, n = 343) the signs of endometritis and/or inflammatory processes in other pelvic organs were present. Finally, in 5.4% (n = 110) of cases, chronic pyelonephritis was diagnosed.
Based on the results of clarifying investigations, individual treatment was prescribed. After treatment completion, control ELI-P-Complex testing revealed full normalization of test parameters in 35.9% (n = 733) of women and improvement of the scores up to the values recommended for pregnancy planning in 47% (959) of patients. In 17.1% of cases (349 women), no clear improvement of ELI-P-Complex test scores was achieved.
Women from Group В (n = 2310) were not examined using ELI-P-Complex method prior to the pregnancy, and their care was conducted according to the uniform common regimens of preconception care, recommended by NICE [
In the first, second, and third trimesters of pregnancy, all Group A patients underwent additional ELI-P- Complex testing. In a majority of cases (94.4%), test scores fluctuated only slightly (±12%) compared to the values reported after preconception care shortly before pregnancy onset. Only 3.7% (n = 73) of pregnant women experienced significant (>12%) changes in the immune reactivity parameters; in 63 (3.2%) of them, changes were transient and were detected during acute respiratory diseases.
After onset of pregnancy, the patients from Group B also underwent ELI-P-Complex testing during the first, second, and third trimesters. Deviations of ELI-P-Complex test scores in Group B women were similar to those observed in Group A women prior to their preconception care. Only 130 (6.5%) pregnant women from Group B had normal ELI-P-Complex test scores on the first examination (in the first trimester of pregnancy), while abnormal decrease/increase in total immune reactivity level or abnormal changes of a-Abs of certain specificity were detected in 93.5% (n = 1868) of cases. During the second trimester, normalparameters were observed already in 16.2% of Group В women, and in 24.4% during the third trimester. However, positive changes in ELI- P-Complex test scores over time during the pregnancy course are relative and most possibly are related to the sequential drop-out of women (pregnancy loss) whose reproductive health was especially poor. Furthermore, therapeutic measures conducted for certain complications affected the improvement of ELI-P-Complex test scores as well.
Summary data concerning peculiarities of pregnancy course and condition of the newborns delivered by women from groups A and B are presented in Tables 2-4.
Pregnancy complications | Group А (n = 1971) | Group B (n = 1998) | P |
---|---|---|---|
First trimester | |||
Threatened miscarriage | 150 (7.6%) | 1746 (87.4%) | Р < 0.01 |
Cervical incompetence | 63 (3.2%) | 116 (5.8%) | Р < 0.01 |
Second trimester | |||
Threatened miscarriage | 71 (3.6%) | 957 (47.9%) | Р < 0.01 |
Pre-eclampsia | 51 (2.6%) | 106 (5.3%) | Р < 0.01 |
Placentitis | 16 (0.8%) | 144 (7.2%) | Р < 0.01 |
Intrauterine hypoxia | 73 (3.7%) | 703 (35.2%) | Р < 0.01 |
Third trimester | |||
Threatened premature labor | 34 (1.7%) | 537 (26.9%) | Р < 0.01 |
Pre-eclampsia | 71 (3.6%) | 204 (10.2%) | Р < 0.01 |
Fetal malformation | - | 10 (0.5%) | Р < 0.01 |
Intrauterine growth restriction | 55 (2.8%) | 186 (9.3%) | Р < 0.01 |
Intrauterine hypoxia | 93 (4.7%) | 430 (21.5%) | Р < 0.01 |
Polyhydramnios | 18 (0.9%) | 44 (2.2%) | Р < 0.01 |
Oligohydramnios | 37 (1.9%) | 56 (2.8%) | Р > 0.05 |
Total pregnant women with complications | 395 (20%) | 1773 (88.7%) | Р < 0.01 |
Pregnancy outcome | Group А (n = 1971) | Group B (n = 1998) | P |
---|---|---|---|
Full term birth | 1734 (88%) | 1237 (61.9%) | Р < 0.01 |
Premature birth | 17 (0.9%) | 224 (11.2%) | Р < 0.01 |
Miscarriage in the first trimester | 169 (8.6%) | 327 (16.4%) | Р < 0.01 |
Miscarriage in the second trimester | 32 (1.6%) | 112 (5.6%) | Р < 0.01 |
Fetal death (stillbirth) | - | 44 (2.2%) | Р < 0.01 |
Missed miscarriage | 7 (0.3%) | 28 (1.4%) | Р < 0.01 |
Anembryonic pregnancy (blighted ovum) | 12 (0.6%) | 26 (1.3%) | Р < 0.05 |
Total adverse pregnancy outcomes | 237 (12%) | 761 (38.1%) | Р < 0.01 |
Newborn’s health state | Group А (n = 1751) | Group B (n = 1461) | P |
---|---|---|---|
Normal (Apgar score ≥ 7) | 1543 (88.1%) | 735 (50.3%) | Р < 0.01 |
Mild perinatal asphyxia | 106 (6.1%) | 279 (19.1%) | Р < 0.01 |
Severe perinatal asphyxia | 13 (0.7%) | 27 (1.8%) | Р < 0.01 |
Intrauterine growth restriction | 66 (3.8%) | 118 (8.1%) | Р < 0.01 |
Premature infant (low birth weight) | 17 (1%) | 224 (15.3%) | Р < 0.01 |
Congenital malformations | 6 (0.3%) | 74 (5.1%) | Р < 0.01 |
Early death cases (at the first 2 wks) | - | 4 (0.3%) | Р < 0.05 |
Total healthy newborns | 1543 (88.1%) | 735 (50.3%) | Р < 0.01 |
Obtained data indicate that normal pregnancy development was significantly more often observed in Group A women, while any kind of unsatisfactory pregnancy outcomes as well as disorders in the health state of the newborns were significantly more often revealed in Group B women.
Calculations of positive predictive value (PPV), sensitivity and specificity of ELI-P-Complex, as well as relative risk of pregnancy complications, adverse pregnancy outcome, and health state of the newborns are presented in
Positive predictive value (PPV) of ELI-P-Complex for prediction of pregnancy complication:
True Positive―Women from 2 subgroups with pregnancy complications.
False Positive―Women from 2 subgroups without pregnancy complications.
Sensitivity and Specificity of ELI-P-Complex for prediction of pregnancy complication:
True Positive―Women from 2 subgroups with pregnancy complications.
False Negative―Women from 1 subgroup with pregnancy complications.
Positive predictive value (PPV), sensitivity and specificity | ||
---|---|---|
Group 1. Women with deviations of immune reactivity in one or more parameters of ELI-P-Complex (n = 2153) | 257 + 1763 | 133 |
Group 2. Women with normal results of ELI-P-Complex (n = 1816) | 148 | 1403 + 145 + 120 |
Relative risk (RR) for pregnancy complications | ||
Group 1. Women with deviations of immune reactivity in one or more parameters of ELI-P-Complex (n = 2153) | 257 + 1763 | 28 + 105 |
Group 2. Women with normal results of ELI-P-Complex (n = 1816) | 127 + 11 + 8 | 1403 + 145 + 122 |
Relative risk (RR) for adverse pregnancy outcome | ||
Group 1. Women with deviations of immune reactivity in one or more parameters of ELI-P-Complex (n = 2153) | 120 + 753 | 165 + 1115 |
Group 2. Women with normal results of ELI-P-Complex (n = 1816) | 108 + 9 + 8 | 1422 + 147 + 122 |
Relative risk (RR) for newborns health state | ||
Group 1. Women with deviations of immune reactivity in one or more parameters of ELI-P-Complex (n = 1549) | 714 + 109 | 620 + 106 |
Group 2. Women with normal results of ELI-P-Complex (n = 1663) | 87 + 12 + 12 | 1297 + 140 + 115 |
True Negative―Women from 3 subgroups without pregnancy complications.
False Positive―Women from 1 subgroup without pregnancy complications.
Relative Risk (RR) for pregnancy complications
a―Positive (bad) outcome (Group 1), b―Negative (good) outcome (Group 1), c―Positive (bad) outcome (Group 2), d―Negative (good) outcome (Group 2).
Relative Risk (RR) for adverse pregnancy outcome
a―Positive (bad) outcome (Group 1), b―Negative (good) outcome (Group 1), c―Positive (bad) outcome (Group 2), d―Negative (good) outcome (Group 2).
Relative Risk (RR) for newborns’ health state
a―Positive (bad) outcome (Group 1), b―Negative (good) outcome (Group 1), c―Positive (bad) outcome (Group 2), d―Negative (good) outcome (Group 2).
Diagnostics with ELI-P-complex test can only be understood clearly realizing that auto-antibodies are always present in the body of any healthy person, and their values vary within certain normal ranges [
Our study, as well as the previous research [
Provided that main etiologic factors impairing the function of female reproductive system are eliminated, complete normalization or significant improvement of the immune reactivity parameters of the embryotropic antibodies system is observed [
Earlier [
Not only immune activation but immune suppression as well can lead to pregnancy disorders. Thus, according to Makarov and Osipova [
Violations of intrauterine development conditions caused by changes in production of maternal a-Abs are associated with the death of the embryo or fetus (although not in all cases); however, they almost always negatively affect the child’s health state. In accordance to observations by Kluchnikov and Zamaleeva, if children were born to women with the normal parameters of ELI-P-Complex method, at least 70% of them were evaluated as practically healthy at ages 4 - 6 years old. On the contrary, no more than 15% children were evaluated as practically healthy if they were born to women with steadily deviated parameters of serum a-Abs [
It should be noted that a threatened pregnancy loss was observed in 1746 (87.4%) patients from Group B in the first trimester of pregnancy and in 957 (47.9%) patients during the second trimester; thus, 1660 (83.1%) pregnant women were treated in the in-patient settings. At the same time, threatened pregnancy loss in patients who underwent preconception care (Group A) was observed during the first and second trimesters in 150 (7.6%) and 71 (3.6%) patients respectively; moreover, only 203 (10.3%) (Р < 0.01) of them required hospitalization and received in-patient treatment. This is confirmed by the data from Liza Osipenko study [
Finally, it should be noted that impaired ELI-P-Complex test scores, despite the hospitalization and conducted treatment during the whole gestational period, increased the risk of adverse pregnancy outcome by 6 times (RR = 5.8908) and the risk of giving birth to an unhealthy child by 8 times (RR = 7.9601) as compared to a group of patients with normal ELI-P-Complex test scores.
In summary, our study has demonstrated that thorough preconception care using ELI-P-Complex test decreases the risk of recurrent adverse pregnancy outcome. Assessment of serum embryotropic antibodies content with ELI-P-Complex test may serve as an objective criterion of female readiness to give birth to a healthy child as well as a criterion of efficacy and sufficiency of therapeutic measures conducted throughout the period of preconception care in women with a history of adverse pregnancy outcomes. Persistent changes in the antibodies against proteins (regulators of embryogenesis) must be considered an alert signal from the body of a future mother. We believe that ELI-P-Complex test may be recommended for a wide use during the preconception care of women with a history of adverse pregnancy outcomes.
Svetlana G.Tsakhilova,Tatiana E.Sharkovskaya,Olga A.Yakimovich,Aida M.Begizova,Angelina A.Malsagova, (2015) “Eli-P-Complex” Diagnostic Test for Preconception Care in Women with History of Adverse Pregnancy Outcome: A Randomized Multicenter Trial. Advances in Reproductive Sciences,03,81-91. doi: 10.4236/arsci.2015.34010