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Study on Retroplacental Hematomas in Finistère

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ToestandWerving
Sponsors
University Hospital, Brest

Sleutelwoorden

Abstract

Cases with placental abruption will be identified by interrogation of two databases of Brest University Hospital between January 2013 and December 2018. First trimester PAPPA and bhCG levels will be recorded. PlGF levels will be measured in women with an available first trimester serum sample. Histological findings in placentas, course of pregnancies, maternal and fetal characteristics will described and compared between cases with and without placental chronic inflammation.

Omschrijving

Identification of cases:

Placental abruption cases will be identified by interrogation of two databases of Brest University Hospital between January 2013 and December 2018.

The women diagnosed with placental abruption will be first identified by interrogation of the Medical Registry Department (MRD) of Brest University Hospital and of five other maternities of our county between January 2013 and December 2018, using the keyword "placental abruption".

Simultaneously, placental abruption cases will be identified from the Pathology department files of Brest University Hospital using a computerized database (ADICAP system).

Cases of placental abruption included in the study will be clinically defined and will not be only diagnosed by histological examination. All cases will be reviewed by an experienced obstetrician in order to confirm the diagnosis.

Duplicates, medical termination of pregnancy, marginal abruption, placenta previa, cases without histological examination of the placenta, histological cases without compatible clinical signs and cases from an unselected maternity will be excluded.

Women identified with placental abruption in the period of study will be sent an information letter explaining the study and its purpose. Women who express their opposition to participate to the study will be excluded.

Clinical parameters:

The following data will be recorded from medical files on a computerized database: baseline maternal characteristics including preconceptional Body Mass Index (BMI), tobacco use, drug use (cocaine, cannabis, buprenorphine) medical history (chronic hypertension, chronic nephropathy, diabetes, cardiovascular disease, autoimmune disease, previous venous thromboembolism), blood and rhesus group, obstetrical history, especially past vasculoplacental disorder and past placental abruption, age at delivery. The following pregnancy characteristics will also be collected: method of conception, medication during pregnancy (in particular aspirin and low molecular-weight heparin (LMWH)), gestational diabetes, premature rupture of membrane, pre-eclampsia (according to the American College of Obstetricians and Gynecologists' definition published in 2013, term at pre-eclampsia diagnosis, term at delivery and method of delivery, postpartum complications including postpartum hemorrhage (defined by a blood loss > 500 ml, whatever the mode of delivery), disseminated intravascular coagulation (DIVC), thromboembolic event after delivery and before hospital discharge, intensive care admission and length of stay.

The following fetal characteristics will be recorded: presence and term at diagnosis of intrauterine growth restriction (IUGR), stillbirth, birthweight and sex of the newborn. IUGR will be defined according to the 2013 French College of Obstetricians and Gynecologists guidelines by an estimated fetal weight below the 10th percentile using locally-accepted curve (AUDIPOG) associated with signs of fetal growth pathological restriction.

Placental parameters:

Histopathological examination of the placentas had been performed by two senior perinatal pathologists at Brest University Hospital. Histological findings were recorded by interrogation of the pathology computerized database APIX V7.

Placentas were fixed in 4% buffered formalin. Standard sampling of three blocks in the central area was performed and slides were Hematoxylin, Eosin and Saffron (HES) stained.

Recorded macroscopic findings will correspond to the following items: placenta weight, fetoplacental weight ratio, placental abruption, abnormal placental set-up (only circumvallation), abnormal umbilical cord (villamentous implantation, thin umbilical cord with < 0,8 cm in diameter, presence of a knot), presence and number of placental infarcts, intervillous thrombi and thrombi in a vessel of the chorionic plate affecting ≥ one third of the placental surface.

Recorded microscopic lesions will correspond to the following items according to Amsterdam consensus: maternal vascular malperfusion lesions such as microscopic infarcts, decidual arteriopathy, abnormal villous maturation (hypermature villi or villous agglutination), presence of fetal vascular malperfusion signs such as obliterative fetal vasculopathy or avascular villi, chorangiosis and erythroblastosis, excessive fibrin deposition, chronic inflammation such as villitis or chronic intervillositis of unknown etiology, chronic chorioamniotitis or chronic deciduitis, acute inflammation such as acute villitis, acute chorioamniotitis or funiculitis.

Biological parameters:

First trimester Down syndrome screening results will be collected for each pregnancy.

First trimester pregnancy associated plasma protein-A (PAPP-A) and β-human chorionic gonadotrophin (βhCG) levels had been measured in international unit/liter and converted to multiples of the median (MoM) using the crown-rump length or biparietal diameter measurement when the blood sample was obtained as an estimate of gestational age.

Available blood samples collected at the end of first trimester of pregnancy (between 11 weeks of gestation (WG) and 13+6 WG) for Down syndrome screening stored at -20°C in Biochemistry department of Brest University Hospital will be used for Placental Growth Factor (PlGF) quantification. Measurements will be done with the automated B.R.A.H.M.S KRYPTOR compact PLUS system (B.R.A.H.M.S PlGF plus KRYPTOR: Thermo Fisher Scientific, Hennigsdorf, Berlin) according to the manufacturer's instructions described elsewhere. PlGF levels will be expressed in pg/ml.

Informed written consents were obtained from women whose blood samples had been collected at the end of first trimester.

Datums

Laatst geverifieerd: 10/31/2019
Eerste ingediend: 11/03/2019
Geschatte inschrijving ingediend: 11/13/2019
Eerst geplaatst: 11/18/2019
Laatste update ingediend: 11/13/2019
Laatste update geplaatst: 11/18/2019
Werkelijke startdatum van het onderzoek: 09/09/2019
Geschatte primaire voltooiingsdatum: 04/09/2020
Geschatte voltooiingsdatum van het onderzoek: 04/09/2020

Conditie of ziekte

Placental Abruption
Placenta Diseases

Fase

-

Armgroepen

ArmInterventie / behandeling
Cases with placental abruption
Cases of placental abruption included in our study will be clinically defined and will not be only diagnosed by histological examination. All cases will be reviewed by an experienced obstetrician in order to confirm the diagnosis.

Geschiktheidscriteria

Leeftijden die in aanmerking komen voor studie 18 Years Naar 18 Years
Geslachten die in aanmerking komen voor studieFemale
BemonsteringsmethodeNon-Probability Sample
Accepteert gezonde vrijwilligersJa
Criteria

Inclusion Criteria:

- Pregnant women

- who had a placental abruption (clinically defined)

- with an available placental histological examination

- in one of 5 maternities of our county (Finistère, France)

- between January 2013 and December 2018.

Exclusion Criteria:

- Medical termination of pregnancy

- marginal abruption

- placenta previa

- cases without histological examination of the placenta

- histological cases without compatible clinical signs

- cases from an unselected maternity.

Resultaat

Primaire uitkomstmaten

1. Histological findings in placentas n°1 [through study completion, an average of one year]

placenta weight

2. Histological findings in placentas n°2 [through study completion, an average of one year]

presence of an histologic placental abruption

3. Histological findings in placentas n°3 [through study completion, an average of one year]

presence of an abnormal placental set-up

4. Histological findings in placentas n°4 [through study completion, an average of one year]

presence of an abnormal umbilical cord

5. Histological findings in placentas n°5 [through study completion, an average of one year]

presence of thrombi in the chorionic plate or intervillous thrombi

6. Histological findings in placentas n°6 [through study completion, an average of one year]

presence of maternal vascular malperfusion lesions such as macroscopic or microscopic infarcts, decidual arteriopathy or abnormal villous maturation

7. Histological findings in placentas n°7 [through study completion, an average of one year]

presence of fetal vascular malperfusion signs such as obliterative fetal vasculopathy or avascular villi

8. Histological findings in placentas n°8 [through study completion, an average of one year]

presence of chorangiosis or erythroblastosis

9. Histological findings in placentas n°9 [through study completion, an average of one year]

presence of excessive fibrin deposition

10. Histological findings in placentas n°10 [through study completion, an average of one year]

presence of chronic inflammation such as villitis or chronic intervillositis of unknown etiology, chronic chorioamniotitis or chronic deciduitis

11. Histological findings in placentas n°11 [through study completion, an average of one year]

presence of acute inflammation such as acute chorioamniotitis or funiculitis

Secundaire uitkomstmaten

1. Maternal first trimester biological markers n°1 [through study completion, an average of one year]

PAPPA

2. Maternal first trimester biological markers n°2 [through study completion, an average of one year]

Beta HCG

3. Maternal first trimester biological markers n°3 [through study completion, an average of one year]

PlGF

4. Course of the pregnancies n°1 [through study completion, an average of one year]

single or twin pregnancy

5. Course of the pregnancies n°2 [through study completion, an average of one year]

use of aspirin or heparin during pregnancy

6. Course of the pregnancies n°3 [through study completion, an average of one year]

occurrence of pre-eclampsia

7. Course of the pregnancies n°4 [through study completion, an average of one year]

occurrence of IUGR

8. Course of the pregnancies n°5 [through study completion, an average of one year]

occurrence of stillbirth

9. Course of the pregnancies n°6 [through study completion, an average of one year]

occurrence of premature rupture of membrane

10. Course of the pregnancies n°7 [through study completion, an average of one year]

occurrence of gestational diabetes

11. Course of the pregnancies n°8 [through study completion, an average of one year]

term at delivery

12. Course of the pregnancies n°9 [through study completion, an average of one year]

mode of delivery

13. Course of the pregnancies n°10 [through study completion, an average of one year]

occurrence of disseminated intravascular coagulation

14. Course of the pregnancies n°11 [through study completion, an average of one year]

occurrence of postpartum haemorrhage

15. maternal characteristics n°1 [through study completion, an average of one year]

parity

16. maternal characteristics n°2 [through study completion, an average of one year]

previous vasculoplacental disorder

17. maternal characteristics n°3 [through study completion, an average of one year]

BMI before pregnancy

18. maternal characteristics n°4 [through study completion, an average of one year]

age at delivery

19. maternal characteristics n°5 [through study completion, an average of one year]

Tobacco use and drug use

20. maternal characteristics n°6 [through study completion, an average of one year]

chronic hypertension or chronic nephropathy

21. maternal characteristics n°7 [through study completion, an average of one year]

diabetes

22. maternal characteristics n°8 [through study completion, an average of one year]

APL syndrome or SLE

23. maternal characteristics n°9 [through study completion, an average of one year]

previous VTE event

24. maternal characteristics n°10 [through study completion, an average of one year]

blood group

25. maternal characteristics n°11 [through study completion, an average of one year]

mode of conception

26. fetal characteristics n°1 [through study completion, an average of one year]

newborn weight

27. fetal characteristics n°2 [through study completion, an average of one year]

sex

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