Predictors of Pregnancy Outcome In SLE and APS

SLE 和 APS 妊娠结局的预测因素

• 批准号: 7924636
• 负责人: Jane E Salmon
• 金额: $ 126.05万
• 依托单位: HOSPITAL FOR SPECIAL SURGERY
• 依托单位国家: 美国
• 财政年份: 2003
• 资助国家: 美国
• 起止时间: 2003-09-25 至 2013-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7924636
• 关键词: Adult; Angiogenesis Inhibitors; Angiogenic Factor; Animals; Anti-DNA Antibodies; Antibodies; Antiphospholipid Antibodies; Antiphospholipid Syndrome; Autoantibodies; Behavior; Biological Markers; Blood - brain barrier anatomy; Brain; Cessation of life; Child; Classical Complement Pathway; Clinical; Cognitive; Cohort Studies; Collection; Complement; Complement Activation; Complement component C1; DNA; Data; Development; Disease; Endoglin; Enrollment; Equilibrium; Etiology; Event; Exposure to; Fetal Growth; Fetal Growth Retardation; Fetus; Fostering; Functional disorder; Funding; Growth; Habitual Abortion; Heparin; Human; Impaired cognition; Infant; Inflammation; Inflammatory; Injury; Knowledge; Laboratories; Lead; Learning Disabilities; Literature; Lupus; Mediating; Mediator of activation protein; Medical; Modeling; Morbidity - disease rate; Mothers; Mus; N-Methyl-D-Aspartate Receptors; Neuraxis; Neurons; Observational Study; Outcome; PGF gene; Patients; Perinatal Exposure; Phenotype; Placental Growth Factor; Placental Insufficiency; Placentation; Plasma; Play; Pre-Eclampsia; Pregnancy; Pregnancy Complications; Pregnancy Outcome; Pregnancy loss; Premature Birth; Research; Research Infrastructure; Research Personnel; Resources; Risk; Role; Sample Size; Sampling; Spontaneous abortion; Systemic Lupus Erythematosus; Testing; Time; Tissues; Translating; Urine; Vascular Endothelial Growth Factor Receptor; Woman; Work; activation product; behavioral impairment; cohort; complement pathway; effective therapy; fetal; in vivo; injured; meetings; mortality; mouse model; neonatal morbidity; neurotoxicity; new therapeutic target; novel; offspring; pregnancy immunology; pregnant; prevent; primary outcome; prospective; stillbirth

DESCRIPTION (provided by applicant): Pregnancy complications in women with the antiphospholipid syndrome (APS) and/or SLE include recurrent miscarriage, preeclampsia, placental insufficiency, and intrauterine growth restriction (IUGR). The mechanisms leading to placental and fetal injury in vivo are incompletely understood and treatment remains sub-optimal. We have identified complement as an early effector in pregnancy loss and/or IUGR associated with placental inflammation in a mouse model of APS and shown that complement activation causes the release of anti- angiogenic factors and abnormal placental development. The PROMISSE Study (Predictors of pRegnancy Outcome: bioMarkers In antiphospholipid antibody Syndrome and Systemic lupus Erythematosus) is a first-time effort to translate our novel findings in mice to humans and determine if elevations of complement split products predict pregnancy complications in patients with antiphospholipid (aPL) antibodies and/or SLE. In the first 4 years of this prospective, observational study of pregnant patients grouped and analyzed according to the presence or absence of aPL antibodies and preexisting SLE, we have enrolled 342 pregnant patients in 7 centers, obtained detailed medical and obstetrical information monthly, and serially collected plasma, serum, DNA, RNA, and urine. Preliminary data suggest that elevated levels of complement activation products antecede and predict poor fetal outcome, consistent with our hypothesis that complement is a proximal mediator of fetal loss and IUGR. We propose to increase our target sample size from 400 to 700 pregnant patients to maintain study power given lower than expected outcome rates, and to leverage the infrastructure and rich collection of patient data and samples by expanding the array of biomarkers and scope of adverse pregnancy outcomes. Specifically, in Aim 1 we will determine whether elevations of split products generated by activation of complement pathways predict poor fetal and/or maternal outcome in patients with aPL antibodies and/or SLE and, in Aim 2, whether the balance of circulating angiogenic and antiangiogenic factors predicts preeclampsia or delivery of IUGR infants. In Aim 3, a new direction, we will use the PROMISSE cohort to affirm in humans our recent findings in mice, that certain anti-DNA antibodies cross-react with N-methyl D- aspartate receptors (NMDAR) and cause neuronal death with ensuing cognitive and behavioral impairment. We propose to quantitate anti-NMDAR antibody levels throughout pregnancy in PROMISSE SLE patients and test the hypothesis that in utero exposure to maternal anti-NMDAR antibodies alters behavior and cognitive development in offspring by evaluating cortical function tasks in 12 month and 3.5 year old children. This competitive renewal and extension of the PROMISSE Study provides an outstanding opportunity to translate knowledge from mouse models to patients, define pathogenic mechanisms, identify predictors of poor pregnancy outcome in APL and/or SLE, and define novel therapeutic targets to prevent such outcomes.Patients with systemic lupus erythematosus (SLE) and/or antiphospholipid (aPL) antibodies are at increased risk for miscarriage, preeclampsia and fetal growth restriction - major causes of maternal, fetal, and neonatal morbidity and mortality in the US and worldwide - whose etiology and mechanism remain unknown and for which therapy is limited. In addition to causing placental dysfunction, maternal autoantibodies may also directly impair fetal brain development. Identification of biomarkers that predict poor pregnancy outcome in these patients will elucidate mechanisms of disease, define targets for treating patients, and generate clinically applicable indicators to permit initiation of interventional trials in patients at greatest risk for pregnancy complications.

描述（由申请人提供）： 抗磷脂综合征（APS）和/或SLE妇女的妊娠并发症包括复发性流产、先兆子痫、胎盘功能不全和宫内生长受限（IUGR）。导致体内胎盘和胎儿损伤的机制尚不完全清楚，治疗仍不理想。我们已经在APS的小鼠模型中鉴定出补体作为与胎盘炎症相关的妊娠丢失和/或IUGR的早期效应物，并表明补体激活引起抗血管生成因子的释放和异常胎盘发育。PROMISSE研究（Predictors of pRegnancy Outcome：bioMarkers In antiphospholipid antibody Syndrome and Systemic lupus Erythematosus）是首次尝试将我们在小鼠中的新发现转化为人类，并确定补体裂解产物升高是否可预测抗磷脂（aPL）抗体和/或SLE患者的妊娠并发症。在这项前瞻性、观察性研究的前4年，根据是否存在aPL抗体和既存SLE对妊娠患者进行分组和分析，我们在7个中心招募了342例妊娠患者，每月获得详细的医疗和产科信息，并连续收集血浆、血清、DNA、RNA和尿液。初步数据表明，补体激活产物水平升高预示胎儿预后不良，这与我们的假设一致，即补体是胎儿丢失和IUGR的近端介质。我们建议将我们的目标样本量从400例增加到700例妊娠患者，以保持研究能力，因为结局率低于预期，并通过扩大生物标志物阵列和不良妊娠结局的范围来利用基础设施和丰富的患者数据和样本收集。具体而言，在目标1中，我们将确定补体途径激活产生的裂解产物升高是否预测aPL抗体和/或SLE患者的胎儿和/或母体结局不良，在目标2中，循环血管生成和抗血管生成因子的平衡是否预测先兆子痫或IUGR婴儿的分娩。在目标3中，一个新的方向，我们将使用PROMISSE队列在人类中证实我们最近在小鼠中的发现，即某些抗DNA抗体与N-甲基D-天冬氨酸受体（NMDAR）交叉反应，并导致神经元死亡，随后出现认知和行为障碍。我们建议在PROMISSE SLE患者的整个妊娠期间定量测定抗NMDAR抗体水平，并通过评估12个月和3.5岁儿童的皮质功能任务来检验子宫内暴露于母体抗NMDAR抗体会改变后代行为和认知发育的假设。PROMISSE研究的这种竞争性更新和扩展提供了一个绝佳的机会，可以将小鼠模型的知识转化为患者，确定致病机制，确定APL和/或SLE不良妊娠结局的预测因子，并确定新的治疗靶点以预防此类结局。系统性红斑狼疮（SLE）和/或抗磷脂（aPL）抗体患者流产的风险增加，先兆子痫和胎儿生长受限--美国和世界范围内母体、胎儿和新生儿发病率和死亡率的主要原因--其病因和机制仍不清楚，治疗也有限。 除了引起胎盘功能障碍外，母体自身抗体还可能直接损害胎儿脑发育。 鉴定预测这些患者不良妊娠结局的生物标志物将阐明疾病机制，确定治疗患者的目标，并产生临床适用的指标，以允许在妊娠并发症风险最高的患者中启动干预性试验。