| Study | Country Study period Study design |
Data source | Exposure definition | Non-exposure definition | Exposition period | Sample size (exposed/unexposed) Or (case / control) |
Remarks | Risk of bias |
|---|---|---|---|---|---|---|---|---|
|
Howren 2020 |
Canada 2002 - 2012 retrospective cohort |
Three administrative health data holdings in British Columbia (BC), Canada, namely Population Data BC, PharmaNet, and the BC Perinatal Database Registry (BCPDR), linked to create a population-based pregnancy cohort. | Pregnant women with rheumatic diseases who filled at least one prescription of methotrexate in preconception (90 days prior to the date of conception) or during pregnancy (i.e., from conception to delivery). (This is a subgroup of exposure among the one considered). |
unexposed, sick
Pregnancies in women with rheumatic diseases without filled prescriptions for conventional synthetic disease modifying anti-rheumatic drugs (csDMARDs) during aforementioned perinatal windows of interest. |
1st trimester, during pregnancy (anytime or not specified), preconceptional for kinetic reason | 24 / 6064 | Each pregnancy can be exposed to more than one category of csDMARDs. | |
| PharmaNet captures complete information on all drug prescriptions dispensed including drug identification number, dispensation date, dispensation quantity, dosage, and duration. | ||||||||
|
Matsui 2003 |
Japan 1974 - 2000 retrospective cohort |
Chiba University Hospital, Japan | Pregnancies in women initially treated with methotrexate for gestational trophoblastic tumor who conceived less than 6 months after completion of chemotherapy. (This is a subgroup of exposure among the whole exposed group considered in the study). |
unexposed, sick
Pregnancies in women initially treated with chemotherapy for gestational trophoblastic tumor who conceived more than 6 months after completion of chemotherapy. |
preconceptional for kinetic reason | 4 / 115 | 17 (30.4%) of 56 patients initially given MTX had to be switched to other single-agent regimens due to the development of drug resistance and/or toxicity. Drug resistance was defined after at least three consecutive cycles of chemotherapy. | |
| Patients with gestational trophoblastic tumor underwent chemotherapy at Chiba University Hospital. | ||||||||
|
Svirsky 2017 |
Israel 2004 - 2014 retrospective cohort |
Medical records of Assaf Harofe Medical Center in Zerifin. | Women treated with methotrexate injection(s) for ectopic pregnancy who subsequently conceived less than 6 months after treatment. |
unexposed, sick
Women treated with methotrexate injection(s) for ectopic pregnancy who subsequently conceived more than 7 months after treatment (between 7 to ≥24 months). |
preconceptional for kinetic reason | 93 / 133 | There is a two years overlap between this study and an earlier published study by the same author: Svirsky et al., 2009. | |
| Medical records. | ||||||||
|
Svirsky 2009 |
Israel 2000 - 2006 retrospective cohort |
Medical records of Assaf Harofeh Medical Center | Women treated with intramuscular injection of methotrexate (MTX) 50mg/m2 in a single dose for ectopic pregnancy who conceived within 6 months from the last methotrexate (MTX) injection. |
unexposed, sick
Women treated with intramuscular injection of methotrexate (MTX) 50mg/m2 in a single dose) for ectopic pregnancy who postponed conception for more than 6 months after the last methotrexate (MTX) injection. |
preconceptional for kinetic reason | 45 / 80 | Index pregnancy is the one following MTX treatment. In two cases of twin pregnancy only the outcome of the first newborn was considered for statistical analysis. | |
| Computerized medical records and a telephone questionnaire when medical records were insufficients. After reviewing the medical records, the women were divided into two groups (less or more than 6 months). | ||||||||
|
Weber-Schoendorfer (Controls exposed to other treatment, sick) 2014 |
Worldwide (9 countries) 1994 - 2011 prospective cohort |
European Network of Teratology Information Services (ENTIS) and Organization of Teratology Information Specialists (OTIS). | Pregnant women who were exposed to MTX only before conception (i.e., between 10 weeks prior to the last menstrual period and no more than 1 week plus 6 days after the last menstrual period) or after conception (i.e., ≥1 dose 2 weeks after the first day of the last menstrual period). |
exposed to other treatment, sick
Pregnant women with rheumatic/inflammatory diseases who did not take MTX during pregnancy or during the 12 weeks before conception. These women had either been treated with other immunomodulatory drugs or the physician had decided not to prescribe any of these drugs. |
preconceptional for kinetic reason | 324 / 459 | Number of total assessed post-conception MTX-exposed infants not reported for genetic birth defects (so not reported here). | |
| Data on exposure were obtained via structured telephone interviews and/or mailed questionnaires completed by the mother and/or her physicians. | ||||||||
|
Weber-Schoendorfer (Controls unexposed, disease free) 2014 |
Worldwide (9 countries) 1994 - 2011 prospective cohort |
European Network of Teratology Information Services (ENTIS) and Organization of Teratology Information Specialists (OTIS). | Pregnant women who were exposed to MTX only before conception (i.e., between 10 weeks prior to the last menstrual period and no more than 1 week plus 6 days after the last menstrual period) or after conception (i.e., ≥1 dose 2 weeks after the first day of the last menstrual period). |
unexposed, disease free
Pregnant women identified through teratology information service centers during spontaneous consultations for other conditions or exposures. Not affected by rheumatic/inflammatory diseases and were not taking any immunomodulatory drugs during pregnancy. |
preconceptional for kinetic reason | 324 / 1107 | Number of total assessed post-conception MTX-exposed infants not reported for genetic birth defects (so not reported here). | |
| Data on exposure were obtained via structured telephone interviews and/or mailed questionnaires completed by the mother and/or her physicians. | ||||||||
| Study | Country Study period Study design |
Data source | Case | Control | Exposition | Exposition period | Sample size (exposed/unexposed) Or (case / control) |
Remarks | Risk of bias |
|---|---|---|---|---|---|---|---|---|---|
|
Dawson 2014 |
USA 1997 - 2009 case control |
National Birth defects Prevention Study (NBDPS). | Infants with major birth defects identified through population-based surveillance systems. | Live-born infants with no major birth defects selected at random from the same ascertainment area as case infants. | Computer-assisted telephone interview which included detailed questions concerning exposures that occurred from 3 months prior to conception through the end of the pregnancy. Mothers were interviewed between 6 weeks and 24 months after their EDD. | 1st trimester, 2nd and/or 3rd trimester, 3 months (or more) before pregnancy or during pregnancy, preconceptional for kinetic reason | 27623 / 10113 | Infants with birth defects with a known etiology, including those with recognized chromosomal syndromes or single-gene disorders, are excluded. The indication for methotrexate use was not reported in most cases. | |
| A clinical geneticist and a pediatrician trained in cardiology review the abstracted clinical records for each case infant. Clinical records for control infants were not available for review. | |||||||||
Risk of bias: : NA; : low; : moderate; : serious; : critical; : unclear;
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