Table 3.
Publication details | Number of participants Indication |
Dose regimen in mU unless otherwise stated (converted from original units) Total or maximum dose Duration Sampling regimen |
Maternal plasma oxytocin levels, pg/mL, mean ± SEM or SD (converted from original units) Important findings |
Oxytocin assay Comments Other reported data |
---|---|---|---|---|
Single dose IV bolus before labour | ||||
Fuchs et. al. (1991) Oxytocin secretion and human parturition: pulse frequency and duration increase during spontaneous labor in women |
18 women Experimental study of bolus SOT in late pregnancy |
Dose regimen: Single IV bolus of 2, 4, 8 or 16 mU Total dose: 2, 4, 8 or 16 mU Sampling regimen: Baseline and at 1, 2, 3, 4, 5 and 10 min |
Results: (Estimated from Fig. 5) Range, pg/mL (μU/mL) Basal (late pregnancy) 0.5–0.7 pg/mL (0.3–0.4 μU/mL) With SOT infusion 0.8–1.7 pg/mL (0.5–1.0) peak Important findings: Dose-dependent rise at 1–2 min at doses 4 mU or higher Decline to approx. Basal over 10 min |
Assay: RIA Comments: Levels similar to spontaneous pre-labour pulses, as measured in this study Other reported data: Contraction pattern and oxytocin levels Number of contractions following the bolus correlated with mean oxytocin peak levels |
Intravenous infusion for labour induction or augmentation: studies with dose-response data and findings | ||||
Amico et. al. (1984) Studies of oxytocin in plasma of women during hypocontractile labor |
11 women Labour augmentation with SOT |
Dose regimen: IV infusion 1 mU/min increased by 1 mU/min every 40 min until ‘adequate contractility’ up to 4 mU/min Maximum dose: Mean 3.4 ± 0.7 mU/min Range 1–8 mU/min Sampling regimen: Baseline and every 20 min until 60–100 min after final infusion rate increase |
Results: (Estimated from Fig. 4) Mean ± SEM, pg/mL (μU/mL) Basal (in labour) 1.7 ± 0.52 pg/mL (1.0 ± 0.31) μU/ml) With SOT infusion 2.7 ± 0.5 (1.6 ± 0.3) at 1 mU/min 3.8 ± 0.7 (2.3 ± 0.4) at 2 mU/min 4.8 ± 1.1 (2.9 ± 0.7) at 3 mU/min 6.3 ± 1.5 (3.8 ± 0.9) at 4 mU/min Important findings: Steady-state oxytocin levels reached 40 min after SOT dose Linear dose-dependent rise (r2 = 0.99) |
Assay: RIA RIA assay giving very low basal levels Comments: Doubling infusion rate approx doubled oxytocin levels Other reported data: Oxytocin metabolic clearance rate (MCR) 11–32.5 (mean 17.3) mL/kg/min SOT administered to 4 men at 125 mU/min 1.3 pg/mL (0.76 μU/mL) basal 188 (112.5) at 60 min Linear dose-dependent rise Steady state oxytocin levels at 30 min Oxytocin MCR 25–34 (mean 17.6) mL/kg/min SOT half-life: 12.3–17.4 min Data from this study also published in Seitchik et al. (1984) |
Amico et. al. (1986) The plasma of pregnant women contains a novel oxytocin-vasotocin-like peptide. |
4 women Labour augmentation with SOT |
Dose regimen: IV infusion 1 mU/min increased 1 mU/min every 40 minutes Maximum dose: 4 mU/min Sampling regimen: Baseline, every 20 min until 60 min after increase to maximum dose |
Results: (Estimated from Fig. 1) Assay Ab-1 Range, pg/mL (μU/mL) 13–25 pg/mL (8–15 μU/mL) basal (in labour) 12–28 (7–17) with SOT infusion Assay Ab-2 Mean pg/mL (μU/mL) < 0.8 pg/mL (< 0.5) basal (in labour) 3.0 (1.8) at 1 mU/min 4.7 (2.8) at 2 mU/min 6.7 (4.0) at 3 mU/min 8.4 (5.0) at 4 mU/min Important findings: Assay Ab-1: No significant rise with infusion Assay Ab-2: Linear dose-dependent rise (p < 0.01) |
Assay: Analysed by 2 different RIA assays: Pitt Ab-1 antiserum Pitt Ab-2 antiserum Comments: Low-dose SOT regimen No rise with Ab-1 assay due to high basal levels vs. clear rise seen with Ab-2 assay Doubling infusion rate approx doubled oxytocin levels (Ab-2 assay) Other reported data: Basal oxytocin in 16 pregnant women at > 36wks (pg/mL ± SE (μU/mL)) Assay Ab-1: 12.9 ± 1.5 (7.7 ± 0.9) Assay Ab-2: 1.5.0 ± 0.3 (0.9 ± 0.2) |
Fuchs et. al. (1983) Oxytocin and the initiation of human parturition. III. Plasma concentrations of oxytocin and 13,14-dihydro-15-keto-prostaglandin F2α in spontaneous and oxytocin-induced labor at term |
15 women Labour induction with SOT 17 women Spontaneous labour, no SOT infusion |
Dose regimen: IV infusion 1-2 mU/min increased every 15 min Maximum dose: Range 1–16 mU/min Sampling regimen: Baseline and just before each increase in infusion rate |
Results: Mean ± SEM, pg/mL With SOT infusion 17.4 ± 4.8 pg/mL pre-induction 21.1 ± 6.4 at 1–3 mU/min 49.1 ± 10.9 at 4–6 mU/min 58.8 ± 9.9 at 7–9 mU/min 110 ± 22.7 at 10–16 mU/min Important findings: Linear dose-dependent rise (p < 0.001) No SOT 15.4 ± 8.7 late pregnancy 19.9 ± 3.1 at < 2 cm 47.2 ± 7.6 at < 4 cm 46.3 ± 7.8 at 4-6 cm 43.0 ± 6.6 at 7-9 cm 45.8 ± 13.6 at 10 cm 45.4 ± 3.9 mean 1st stage |
Assay: RIA Comments: Doubling infusion rate approx doubled oxytocin levels Oxytocin levels below 10 mU/min are within range of levels in women with no SOT |
Furuya et. al. (1988) [Fundamental studies on the measurement of plasma concentration of oxytocin during perinatal period] |
5 women Labour induction with SOT |
Dose regimen: IV infusion 12 mU/min (20 ng/min) increased up to maximum 32 mU/min (53 ng/min) Maximum dose: Range 24-32 mU/min (40–53 ng/min) Sampling regimen: Baseline and with each increase |
Results: (Estimated from Fig. 7) Mean ± variation, pg/mL Infusion rate mU/min (ng/min) Basal (pre-labour) 2 pg/mL With SOT infusion 8 ± 5 at 12 mU/min (20 ng/min) 17 ± 5 at 16 mU/min (26) 19 ± 8 at 20 mU/min (33) 38 ± 14 at 24 mU/min (40) 55 ± 6 at 32 mU/min (53) Important findings: Fig. 7 shows approx. Linear dose-response curve, although no statistics provided |
Assay: RIA Comments: No control group Dose intervals not stated Variation statistic not stated Doubling infusion rate approx tripled oxytocin levels Data at highest infusion rate based on 3 samples Other reported data: Oxytocin with breastfeeding (n = 1, estimated from Fig. 8) 2.5 basal 14.3 peak at 20 min Peak levels similar to SOT infusion at 16 mU/min |
Perry et. al. (1996) The pharmacokinetics of oxytocin as they apply to labor induction |
10 women Labour induction with SOT |
Dose regimen: 6 mU/min, increasing by 6 mU/min every 40 min to max 42 mU/min Maximum dose: Mean maximum dose: 22.8 ± 3.6 mU/min Sampling regimen: Baseline (in labour) and at intrauterine pressures of; 100–150, 150–200 and > 200 Montevideo units All samples taken > 40 min after change of SOT infusion rate |
Results: Mean ± SEM, pg/mL Basal (pre-labour) 21.2 ± 0.9 pg/mL With SOT infusion 26.4 ± 1.3 at maximum uterine pressure Important findings: Oxytocin levels correlated with SOT infusion rate (p < 0.001) but not uterine pressure. (Data not provided) |
Assay: RIA Comments: Small increment in oxytocin levels with quite high SOT infusion rates suggests insensitive assay Other reported data: Oxytocin MCR MCR independent of oxytocin levels (p = 0.71) |
Seitchik et. al. (1984) Oxytocin augmentation of dysfunctional labor. IV. Oxytocin pharmacokinetics |
See Amico et al. (1984) | See Amico et al. (1984) | See Amico et al. (1984) | Data from this study also published in Amico et al. (1984) |
Thornton et. al. (1990) Effect of human pregnancy on metabolic clearance rate of oxytocin |
10 women Labour induction with SOT 10 women Administered SOT at 8–10 weeks postpartum (see below) |
Dose regimen (lLabour): IV infusion 10.7 mU/min (17.9ng/min) increased after 30 min to 21 mU/min (35.7 ng/min) Maximum dose: 21 mU/min (35.1 mg/min) ( Postpartum: see below)- italics please Sampling regimen: 6 samples over 60 sec at baseline and 30 min, then 30 min after each infusion rate increase |
Results: Mean ± SEM, pg/mL Infusion rate mU/min (ng/min) With SOT infusion 1.5 ± 0.3 pg/mL basal (pre-labour) 5.0 ± 0.5 at 10.7 mU/min (17.9 ng/min) 8.0 ± 0.9 at 21 mU/min (35.7) Important findings: These oxytocin levels were similar to those in postpartum women who were administered significantly lower SOT doses (see below), suggesting greater metabolism of SOT in pregnancy |
Assay: RIA Comments: Doubling infusion rate approx doubled oxytocin levels Other reported data: Oxytocin MCR MCR independent of concentration and higher in pregnancy vs postpartum (p < 0.001). Plasma oxytocinase activity High oxytocinase activity in pregnancy (2.1 ± 0.02 IU/mL), very low postpartum (< 0.1 IU/mL) |
Intravenous infusion for labour induction or augmentation: sporadic measurements | ||||
Arai T. (1980) The significance of plasma oxytocin in pregnancy and at parturition Publication in Japanese Data obtained from full article translated into English |
14 women Labour induction with SOT 16 women Spontaneous labour, no SOT infusion or other interventions |
Dose regimen: IV infusion Stated as 15 μU/min (=0.015 mU/min, extremely low dose More likely 15 mU/min) Total dose, duration: Not stated Sampling regimen: Before labour During 2nd stage labour |
Results: Mean ± SD, pg/mL (μU/mL) Basal (40 wks gestation) 69.3 ± 17.7 (41.6 ± 10.6) (n = 8) With SOT infusion 120.1 ± 42.8 (71.9 ± 25.6) in labour No SOT 77.0 ± 28.2 (46.1 ± 16.9) in labour Important findings: Mean levels in labour significantly higher with SOT vs no SOT (p < 0.01) |
Assay: RIA Comments: Oxytocin levels in labour with SOT approx double vs in labour without SOT Other reported data: Oxytocin patterns in a single contraction cycle Reported below Oxytocin levels following prostaglandin induction, pre-labour and in-labour caesarean, and caesarean following SOT treatment in labour (This data to be reviewed in subsequent systematic reviewa) |
De Tina et.al (2019) Oxytocin and Oxytocinase in the Obese and Nonobese Parturients during Induction and Augmentation of Labor |
50 women (25 obese & 25 non-obese) Labour induction with SOT |
Dose regimen: IV infusion Maximum dose: 20 mU/min Total Dose: (mean ± SD) Nonobese women 3.4 ± 1.6 IU Duration: Nonobese women, 397 ± 159 min Sampling regimen: Baseline and 20 min after maximum infusion rate |
Results: Non-obese women with complete data (n = 18) Median (IQR), pg/mL Basal (pre-labour) 351 pg/mL(56, 790) With SOT infusion 463 (15, 791) Important findings: No increase following SOT infusion |
Assay: ELISA ELISA gives higher levels than RIA with different effect patterns Comments: Similar data in obese group, which was analysed separately in this study Low SOT dose (generally insufficient to increase plasma oxytocin) Small oxytocin rise may reflect labour-related release Other reported data: Oxytocin and oxytocinase levels in obese vs. non-obese women Oxytocin levels or total SOT dose not significantly different in obese vs non-obese women Lower initial oxytocinase levels in obese vs non-obese (p = 0.03) |
Husslein et. al. (1983b) Oxytocin and the initiation of human parturition. IV. Plasma concentrations of oxytocin and 13,14-dihydro-15-keto-prostaglandin F2 alpha during induction of labor by artificial rupture of the membranes |
6 Women Labour induction with ROM and later required SOT 16 women Labour induction with ROM, no SOT |
Dose regimen: IV infusion 5 mU/min Started 4–15 hr. after ROM when required Maximum dose: Not stated Sampling regimen: Before ROM, at 15 min and 2 hr., then 2–3 hourly |
Results: Mean ± SEM, pg/mL With SOT infusion (after ROM) 38.3 ± 10.7 pg/mL basal (pre-induction) 59.9 ± 15.4 at 5 hr (3/6 with SOT) 53.0 ± 24.3 at 8 hr (2/3 with SOT) 63.1 ± 9.2 mean all samples No SOT 33.6 ± 7.7 basal (pre-induction) 40.6 ± 11 at 5 hr 32.9 ± 8.1 at 8 hr Important findings: Oxytocin levels significantly increased after vs before SOT infusion |
Assay: RIA Comments: Oxytocin levels in labour with SOT approx double vs in labour without SOT Other reported data: Plasma PGFM (PG metabolite) following SOT infusion: PGFM increased in 6/6 women with successful induction Oxytocin levels following ROM (This data to be reviewed in subsequent systematic reviewa) |
Otsuki et al. (1983) Feto-maternal plasma oxytocin levels in normal and anencephalic pregnancies. |
5 women Labour induction with SOT 6 women Spontaneous labour, no induction or SOT |
Dose regimen: Not stated Maximum dose: Not stated Sampling regimen: Baseline, early labour and 2nd stage |
Results: Mean ± SEM, pg/mL (reported in μU/mL) Basal (pre-induction) 20.7 ± 2.8 pg/mL (12.4 ± 1.7 μU/mL) With SOT infusion 40.7 ± 8.7 (24.4 ± 5.2) early labour 63.1 ± 12.9 (37.8 ± 7.7) 2nd stage No SOT 21.0 ± 3.0 (12.6 ± 1.8) early labour 29.4 ± 6.0 (17.6 ± 3.6) 2nd stage Important findings: SOT significantly higher vs no SOT at 1st (p < 0.05) and 2nd (p < 0.01) stages |
Assay: RIA Comments: Oxytocin levels in labour with SOT approx double vs. in labour without SOT Other reported data: Maternal oxytocin levels in 4 women with anencephalic babies induced with SOT at 32–34 wk 22.4 ± 13.4 pg/mL 2nd stage Other reported data: Newborn UA and UV oxytocin levels with maternal SOT exposure (See Table 4) |
Padayachi et. al. (1988) Serial oxytocin levels in amniotic fluid and maternal plasma during normal and induced labour |
8 women Labour induction with SOT and amniotomy (women allocated alternately with PG induction) 13 women Spontaneous labour, no SOT |
Dose regimen: IV infusion at 2 mU/min increased every 30 min Maximum dose: 32 mU/min Sampling regimen: Collected over 4 min every hr. |
Results: Mean ± SEM, pg/mL (μU/mL) With SOT infusion 5.9 ± 1.0 pg/mL at < 4 cm (3.55 ± 0.62 μU/mL) 10.1 ± 1.3 (6.07 ± 0.78) at 8–10 cm No SOT 6.8 ± 0.65 (4.05 ± 0.39) at < 4 cm 9.2 ± 1.15 (5.48 ± 0.69) at 8–10 cm Important findings: Significant rise during labour with SOT (p < 0.02) |
Assay: RIA Comments: RIA giving very low levels in all groups Slow sampling may average out any peaks of oxytocin |
Pochard & Lutz-Bucher (1986) Vasopressin and oxytocin levels in human neonates. Relationships with the evolution of labour and beta-endorphins |
6 women Labour induction with ‘oxytocic drugs’ 21 women No oxytocic drugs 10 women No oxytocic drugs Fetal distress in labour |
Dose regimen: Not stated Maximum dose: Not stated Sampling regimen: Before expulsive phase |
Results: (Estimated from Fig. 1) Mean, pg/mL Oxytocic drugs 3 pg/mL No oxytocic drugs 2–3 Fetal distress 4 Important findings: No statistically significant differences between any groups. |
Assay: RIA Comments: Oxytocic drugs presumed to be SOT Other reported data: Newborn UA and UV oxytocin with maternal SOT exposure (See Table 4) Maternal plasma and newborn UA and UV AVP (vasopressin) levels No difference between any groups Maternal plasma and newborn UA and UV oxytocin levels with pre-labour caesarean (This data to be reviewed in subsequent systematic reviewa) |
Risberg et. al. (2015) Water balance during parturition and early puerperium: A prospective open trial |
12 women Spontaneous labour, augmentation with SOT for ‘dystocia’(9/12 epidural, 5/12 postpartum SOT) 30 women Spontaneous labour No IV fluids or other medication (14/30 postpartum SOT) 9 women Spontaneous labour IV fluids only (7/9 epidural, 6/9 postpartum SOT) Women who required SOT were randomised to continuous (n = 6) or pulsatile (n = 5) infusions |
Dose regimen: 10 IU/L (10 mU/mL) by continuous (n = 6) or pulsatile (n = 5) infusion: Continuous infusion 15 mL/hr. (2.5 mU/min) increased until adequate contractions (3–5/10 min) Duration: 72–480 min Maximum dose: 120 mL/hr. (20 mU/min) Total dose: 2.5 ± 1.1 IU total Pulsatile infusion 1.8 mL/hr. (0.3 mU/min) increased until adequate contractions Duration: 20–240 min Total dose: 0.4 ± 0.5 IU Postpartum dose: 25 of these women also received 10–30 IU SOT bolus Sampling regimen: Arrival, early 1st stage, early 2nd stage, just after birth and 9, 15, 27 hr. postpartum |
Results: Mean ± SD, pmol/L equivalent to pg/mL With SOT infusion (Includes continuous and pulsatile infusion regimens) 31.3 ± 3.0 at arrival 29.4 ± 3.8 early 1st stage 29.5 ± 2.8 early 2nd stage 32.7 ± 3.3 just after birth 26.3 ± 2.5 9 hr. postpartum 28.8 ± 2.4 15 hr. postpartum 27.3 ± 3.6 27 hr. postpartum No SOT or IV fluids 32.4 ± 3.8 at arrival 20.7 ± 2.7 early 1st stage 29.3 ± 2.9 early 2nd stage 41.5 ± 8.3 just after birth 26.7 ± 1.2 9 hr. postpartum 28.0 ± 1.1 15 hr. postpartum 27.5 ± 1.3 27 hr. postpartum Important findings: Oxytocin concentrations not significantly different with vs without SOT or before vs after parturition |
Assay: ELISA with previous extraction ELISA gives higher levels than RIA with different effect patterns Comments: Very low SOT dosage, especially with pulsatile dosage Multiple sub-groups and co-interventions make interpretation difficult High mean oxytocin just after birth in No SOT group may relate to mother-newborn SSC initiated soon after birth Other reported data: Pulsatile vs continuous SOT infusion Significantly lower total SOT dose (p < 0.05), no difference in labour progress SOT vs. controls SOT-exposed had lower plasma osmolarity at arrival (p < 0.05) and lower sodium (p < 0.01) in late labour AVP vs. controls AVP levels not significantly different between groups |
Seitchik et. al. (1985) Oxytocin augmentation of dysfunctional labor. V. An alternative oxytocin regimen |
10 women Labour augmentation with SOT |
Dose regimen: IV infusion 5 mU/min increased by timed or arithmetic protocol until adequate uterine response Maximum dose: Range 2.3–5.7 mU/min Sampling regimen: Baseline (2 samples 5 min apart), at adequate uterine response, and every 15 min (up to 4 samples) after maintenance dose reached |
Results: Mean ± SD, pg/mL (μU/mL) Basal (in labour) 1.4 ± 0.20 pg/mL (0.83 ± 0.1 μU/mL) With SOT infusion 2.6 ± 0.3 (1.6 ± 0.2) at adequate uterine response 3.0 ± 0.5 (1.8 ± 0.3) at 45 mins 2.8 ± 0.6 (1.7 ± 0.3) at 60 mins Important findings: Oxytocin levels approx doubled from basal at the infusion rate that gave adequate uterine response |
Assay: RIA Comments: Oxytocin levels not analysed in relation to SOT infusion rate Other reported data: Time required to achieve steady-state blood oxytocin levels 40 min after dose increase |
Thornton et. al. (1992) Plasma oxytocin during the first and second stages of spontaneous human labour |
5 women Spontaneous labour, augmentation with SOT 7 women Spontaneous labour, no SOT |
Dose regimen: 4 mU/min increased every 15 min until adequate uterine activity Total dose: Not stated Sampling regimen: Every minute for 15 min in early labour (baseline) and in late 1st stage From onset 2nd stage pushing until birth |
Results: Mean ± SD, pmol/L equivalent to pg/mL U: undetectable With SOT infusion U-4.6 pg/mL early labour U-10.0 late 1st stage No SOT U-6.2 early labour U-4.8 late 1st stage Important findings: Significant oxytocin rise following SOT infusion No significant oxytocin rise in 6/8 controls “Large increase” in oxytocin in 2nd stage in 2/8 women e.g. 27 pmol/L |
Assay: RIA Assay detection limit 1.4 pmol/L Comments: Many samples with undetectable levels No increase during labour despite frequent sampling suggests insensitive assay Oxytocin levels in labour with SOT approx double vs in labour without SOT |
Intravenous infusion for labour induction or augmentation: oxytocin patterns during a single contraction cycle | ||||
Arai T. (1980) The significance of plasma oxytocin in pregnancy and at parturition Publication in Japanese Data obtained from full article translated into English |
14 women Labour induction with SOT 16 women Spontaneous labour, no SOT infusion or other interventions |
Dose regimen: IV infusion Stated as 15 μU/min (=0.015 mU/min, extremely low dose More likely 15 mU/min) Total dose, duration: Not stated Sampling regimen: Sampled 4 times during a single contraction cycle in both 1st and 2nd stages |
Results: Mean ± SD, pg/mL (μU/mL) Basal (40 weeks gestation) 69.3 ± 17.7 pg/mL (32.9 ± 10.6 μU/mL) Oxytocin levels in a single contraction cycle Sampled between, early, at peak and late in contractions: With SOT infusion: Stage 1 (2 samples) 107.9 ± 25.9 (64.6 ± 15.5) between contractions 98.2 ± 33.7 (58.5 ± 20.2) peak Stage 2: 97.2 ± 44.8 (58.2 ± 26.8) between 74.6 ± 1.2 (44.7 ± 0.7) early 102.2 ± 37.7 (61.2 ± 22.6) peak 64.1 ± 8.7 (38.4 ± 5.2) late Important findings: Levels significantly lower between vs. during contraction (Stage 1) No SOT: Stage 1 83.5 ± 17.5 (50.0 ± 10.5) between 70.0 ± 31.9 (41.9 ± 19.1) early 42.9 ± 15.4 (25.7 ± 9.2) peak 55.9 ± 28.4(33.5 ± 17.0) late Stage 2: 85.2 ± 16.4 (51.0 ± 9.8) between 70.0 ± 16.4 (41.9 ± 9.8) early 72.0 ± 29.1 (43.1 ± 17.4) peak 65.0 ± 30.7 (38.9 ± 18.4) late Important findings: Levels significantly lower at peak of contraction vs other times (Stage 1 only, p < 0.02) |
Assay: RIA Comments: Differing patterns, with lowest oxytocin levels between contractions with SOT vs lowest at contraction peak with no SOT Other reported data: Oxytocin levels following prostaglandin induction, pre-labour and in-labour caesarean, and caesarean following SOT treatment in labour (This data to be reviewed in subsequent systematic reviewa) |
Buccal administration | ||||
Dawood et. al. (1980) Plasma oxytocin levels and disappearance rate after buccal Pitocin |
9 women Labour induction or augmentation with SOT |
Dose regimen: Buccal administration 400 IU every 20 min Total dose: 400–2200 IU Sampling regimen: Baseline, at 20–30 min, then hourly |
Results: Range, pg/mL Basal (before SOT) 1.5–107 pg/mL With SOT buccal 6.8–181 peak Important findings: Very variable rise Levels not related to dose |
Assay: RIA Comments: Buccal SOT is no longer used clinically Other reported data: Male subjects (3) given buccal SOT 200–400 IU every 20 min Mean levels 24–32 at 400 IU Still elevated above basal 45 min after administration |
Postpartum intravenous or intramuscular administration | ||||
Ende et.al. (2019) Association of Interindividual Variation in Plasma Oxytocin With Postcesarean Incisional Pain |
18 women Pre-labour caesarean with postpartum IV SOT (all women) |
Dose regimen: (Titrated to effect) Intra-operative dose: 3–35 IU (mean 14.1 ± 8.6 SD) Post-operative dose: 9–31.5 IU (mean 15.5 ± 4.8 SD) Duration: not stated Total dose: 19–48.5 (mean 29.5 ± 9.4 SD) Sampling regimen: I hr. before, then 1 and 24 hr post-caesarean |
Results: Mean ± SD pg/mL (ng/mL) Mean (all women) 335 ± 452 pg/mL Range (Estimated from Fig. A) 1–1200 pre-caesarean (0.001–1.2 ng/mL) 30–1200 (0.03–1.2) 1 hr post-caesarean 4–1100 (0.004–1.1) 24 hr post-caesarean Important findings: Very high interindividual variability Significantly lower oxytocin at 1 and 24 hr. post- vs pre-caesarean (p = 0.001) |
Assay: ELISA ELISA gives higher levels than RIA with different effect patterns Comments: Oxytocin data difficult to interpret Assay did not detect oxytocin rise at 1 hr. despite high intra- and post-operative SOT dose Other reported data: Pain score at 24 hr Significantly lower in women with higher oxytocin levels at 1 and 24 hr. post-caesarean (p = 0.047, p = 0.008 respectively) |
Fuchs et. al. (1982) The origin of circulating 13,14-dihydro-15-keto-prostaglandin F2 alpha during delivery |
10 women Postpartum SOT IV infusion 10 women Postpartum IV infusion without SOT |
Dose regimen: In labour: Some women also received SOT IV infusion 1–8 mU/min, stopped average 50 min before birth Postpartum: 100–150 mU/min starting immediately after birth for 2 hr., infusion rate reduced over time Total postpartum dose: 12–18 IU Sampling regimen: Full dilatation, then 5 min, 30 min and 2 hr. postpartum |
Results: Mean ± SD, pg/mL Basal 18.0 ± 3.2 pg/mL pre-labour With SOT infusion 50.1 ± 9.7 2nd stage 93.4 ± 20.6 5 min postpartum 275 ± 46.5 30 min postpartum 127 ± 22.6 2 hr. postpartum No SOT 50.1 ± 10.7 2nd stage 41.1 ± 11.0 5 min postpartum 29.1 ± 9.7 30 min postpartum 29.4 ± 6.8 2 hr. postpartum Important findings: Postpartum oxytocin significantly higher with vs without SOT at 30 min and 2 hr. (both p < 0.001) |
Assay: RIA Comments: Skin-to-skin contact not recorded Other reported data: PG levels postpartum Significantly higher PG levels at 2 hr. postpartum following postpartum SOT vs no postpartum SOT Data from this study also published in Husslein et al. (1982) |
Gibbens, D et.al (1972) The circulating level of oxytocin following intravenous and intramuscular administration of Syntometrine |
10 W SOT IM 14 W SOT IV 2 W SOT by subcutaneous injection (SC) |
Dose regimen: Single injection at birth of baby’s anterior shoulder Total dose: 5 IU (combined with ergometrine 500 mcg) Sampling regimen: Basal then at varying intervals up to 120 mins: Frequent intervals 0–240 sec after IV (n = 4) |
Results: (Estimated from Fig. 1) Mean, pg/mL Basal: Undetactable in all Intramuscular: 10 at 15 sec 20 at 30 sec 40 at 1 min 50 at 3 min 45 at 6 min 43 at 12 min 18 at 18 min 18 at 30 min 0 at 60 min Intravenous: 35 at 15 sec 330 at 30 sec 550 at 1 min 280 at 3 min 100 at 6 min 70 at 12 min 40 at 18 min 20 at 30 min 0 at 60 min Important findings: Following IM, much lower peak levels vs. IV, with a more sustained elevation |
Oxytocin assay: RIA Max sensitivity reported as 1.5 pg/mL No oxytocinase inhibitor was added, suggesting that some degradation may have occurred Comments: Low basal levels suggests that actual peak levels may be higher than reported Other reported data: IM oxytocin levels Oxytocin first detected at 45 sec (average), still detectable at 60 min in 3/10 IV oxytocin levels Initial rapid fall (initial half-life 3 min) followed by slower disappearance IV levels at 20–220 sec (Fig. 2, n = 2) show peaks around 400–700 pg/mL at 40–80 sec with marked variability and decline to < 100 pg/mL at 220 sec SC oxytocin levels Levels undetectable (n = 1) and very low (39 pg/mL at 30 mins, n = 1) |
Husslein P et.al. (1983a) [Oxytocin- and prostaglandin plasma concentrations before and after spontaneous labor: evidence of involvement of prostaglandins in the mechanism of placental separation]. Publication in German |
See Fuchs et.al (1982) | See Fuchs et.al (1982) | See Fuchs et.al (1982) | Data from this study also published in Fuchs et.al (1982) |
Thornton et. al. (1988) Plasma oxytocin during third stage of labour: comparison of natural and active management |
25 women Postpartum SOT IM 15 women No postpartum SOT |
Dose regimen: Single IM injection of at birth of baby’s anterior shoulder Total dose: 5 IU (combined with ergometrine 500 mcg) Sampling regimen: Every 30 sec for 15 min from crowning of the head |
Results: Mean ± SD, pmol/l equivalent to pg/mL With SOT IM postpartum 3.1 ± 2.0 pg/mL before anterior shoulder 15.9 ± 2.7 after birth Mean peak level 30.5 ± 2.5 No SOT In 9/15 women: 2.4 ± 3.1 before anterior shoulder 2.2 ± 2.2 after birth In 6/15 women: 3.2 ± 2.0 before anterior shoulder 6.4 ± 2.0 after birth Mean peak level 11.6 ± 1.5 Important findings: Significant rise following SOT (p < 0.001) In 6/15 with no SOT, significant rise (p < 0.01) with “remarkably similar” pattern to SOT |
Assay: RIA |
Thornton et. al. (1990) Effect of human pregnancy on metabolic clearance rate of oxytocin |
10 women Administered SOT at 8–10 weeks postpartum (experimental) (SOT also administered in labour- see above) |
Dose regimen: IV infusion 4.3 ng/min (2.6 mU/min) increased after 30 min to 8.5 ng/min (5.1 mU/min) Maximum dose: 8.5 ng/min (5.1 mU/min) Sampling regimen: 6 samples over 60 sec at baseline and 30 min, then 30 min after infusion rate increase |
Results: Mean ± SEM Infusions, mU/min (ng/min) Basal 1.7 ± 0.5 pg/mL With SOT infusion 5.2 ± 0.4 pg/mL at 2.6 mU/min (4.3 ng/min) 8.0 ± 0.3 at 5.0 mU/min (8.5) Important findings: Oxytocin levels postpartum similar to labouring women who were administered significantly higher SOT doses (see above), suggesting greater metabolism of oxytocin in labour |
Assay: RIA Comments: Doubling infusion rate approx doubled oxytocin levels, similar to dose-response elevations seen in labouring women in this study Other reported data: Oxytocin metabolic clearance rate (MCR) MCR independent of concentration and higher in pregnancy vs postpartum (p < 0.001) Plasma oxytocinase activity High in pregnancy (2.1 ± 0.02 IU/mL), very low postpartum (< 0.1 IU/mL) |
Velandia (2012) Parent-Infant Skin-to-Skin Contact Studies |
34 women Pre-labour caesarean Randomised to 25 min newborn SSC with mother or with father Control groups: the parent without SSC All groups Initial 5 min SSC with mother and were returned to mother after 30 min |
Dose regimen: All women received 5 IU SOT IV after birth 19 women also received 50 IU SOT IV infusion over 90–158 min (316–555 mU/min) Sampling regimen: Basal (before surgery) At birth then every 5 min for 45 min, then every 15 min up to 120 min |
Results: (Estimated from Figs. 13, 14, 15) Mean, pM equivalent to pg/mL SOT infusion & SSC (n = 7) 35 pg/mL basal 49 at 10 min 64 at 20 min 49 at 30 min 30 at 40 min 32 at 60 min 53 at 75 min No SOT infusion & SSC (n = 8) 22 basal 26 at 10 min 31 at 20 min 32 at 30 min 29 at 40 min 24 at 60 min 23 at 75 min SOT infusion, no SSC (n = 12) 26 basal 37 at 10 min 37 at 20 min 32 at 30 min 33 at 40 min 31 at 60 min 50 at 75 min No SOT infusion, no SSC (n = 7) 29 basal 32 at 10 min 42 at 20 min 32 at 30 min 31 at 40 min 31 at 60 min 32 at 75 min Important findings: Rise from basal was significant at 20 and 75 min for women with SOT and SSC (p < 0.001) but not for other groups |
Assay: RIA Other reported data: Oxytocin levels postpartum All groups of mothers and fathers with or without SSC had non-significant oxytocin rise over first 60 min, then levels decreased to basal SSC vs no SSC Fathers: no difference in oxytocin with SSC vs no SSC Newborns: Earlier first breastfeed when SSC with mother vs father (p = 0.018) Girls cried more in SSC with mother vs father (p = 0.004) Maternal personality profile at 2 days in relation to SOT and SSC Greatest personality changes on Karolinska Scale of Personality (vs. normative) in women with both SOT and SSC |
Yamaguchi et. al. (2011) Serum oxytocin concentrations in elective caesarean delivery: A randomized comparison of three infusion regimens |
30 women Pre-labour caesarean Randomised to 3 postpartum SOT IV regimens |
Dose regimen: IV infusion started post-op (just after newborn cord clamped) Randomised to: a. 10 IU over 30 min (330 mU/min) b. 10 IU over 3 min (3330 mU/min) c. 80 IU over 30 min (2670 mU/min) Total dose: 10 or 80 IU Sampling regimen: Basal (pre-infusion) 5, 30 and 60 min after initiation of SOT infusion |
Results: Mean ± SD pg/mL (reported in ng/mL) a. 10 IU over 30 min (330 mU/min) 60 ± 20 pg/mL (0.06 ± 0.02) basal 710 ± 270 (0.71 ± 0.270) at 5 min 1170 ± 370 (1.17 ± 0.37) at 30 min 650 ± 260 (0.65 ± 0.26) at 60 min b. 10 IU over 3 min (3330 mU/min) 40 ± 20 (0.04 ± 0.02) basal 1970 ± 650 (1.97 ± 0.65) at 5 min 410 ± 210 (0.41 ± 0.21) at 30 min 360 ± 260 (0.36 ± 0.26) at 60 min c. 80 IU over 30 min (2670 mU/min 70 ± 40 (0.07 ± 0.04) basal 3650 ± 740 (3.65 ± 0.74) at 5 min 6190 ± 1190(6.19 ± 1.19) at 30 min 80 ± 250 (0.08 ± 0.25) at 60 min Important findings: 8-fold higher dose (80 IU vs 10 IU) gives 5-fold higher levels at 5 and 30 min |
Assay: ELISA with extraction ELISA gives higher levels than RIA with different effect patterns Other reported data: Uterine tone: Adequate in all groups, no additional uterotonic drugs required Cardiovascular: No significant changes in blood pressure or heart rate in any group, despite very high SOT dose |
Yuksel et. al. (2016) Immediate breastfeeding and skin-to-skin contact during cesarean section decreases maternal oxidative stress, a prospective randomized case-controlled study |
90 women Pre-labour caesarean Randomised to immediate vs. delayed (1 hour) newborn SSC |
Dose regimen: 5 IU bolus after newborn cord clamped then 20 IU/hour infusion Sampling regimen: Basal (before surgery) 15 mins post-surgery |
Results: Mean (range), pg/mL Delayed SSC 363.3 (187–645) pg/mL at 15 mins Immediate SSC 670.0 (435–890) at 15 mins Important findings: Oxytocin levels significantly higher with immediate vs delayed SSC (p = 0.003) |
Assay: ELISA ELISA gives higher levels than RIA with different effect patterns Comments: All women received SOT Other reported data: Postoperative serum oxidative stress markers: Oxidative stress markers more favourable with immediate vs delayed SSC (p < 0.001), and positively correlated with oxytocin levels (p < 0.001) SSC and pain markers: Women with immediate vs delayed SSC had non-significantly lower pain scores and lower analgesia requirements |
Administration of synthetic oxytocin with later postpartum sampling: exposed vs. unexposed analysis | ||||
Handlin et. al. (2009) Effects of sucking and skin-to-skin contact on maternal ACTH and cortisol levels during the second day postpartum-influence of epidural analgesia and oxytocin in the perinatal period |
See Jonas (2009) | See Jonas (2009) | See Jonas (2009) | (Data from this study also published in Jonas et al. 2009) |
Jonas et. al. (2009) Effects of intrapartum oxytocin administration and epidural analgesia on the concentration of plasma oxytocin and prolactin, in response to suckling during the second day postpartum |
Intrapartum: 8 women Labour augmentation with SOT 14 women Labour augmentation with SOT plus epidural analgesia 20 women Spontaneous labour, no SOT or other interventions All women primiparous |
Dose regimens: SOT IV infusion: Total dose: Median 0.8 IU (1.35 μg) IQR 0.3–1.6 IU (0.53–2.73 μg) SOT IV infusion with epidural (SOT/EDA): Total dose: Median 0.9 IU (1.43 μg) IQR 0.4–1.8 IU (0.74–3.06 μg) Sampling regimen: During breastfeeding at 24–48 hr. postpartum with skin-to-skin contact (SSC) Baseline sample at first latch then 15 samples at 30 sec intervals over first 7.5 min and then 10, 20, 30, and 60 min |
Results: A median of all samples for each woman was calculated, which were combined into group medians Median (IQR), pg/mL SOT/No EDA 156.3 pg/mL (102.0–376.2) basal 176.6 (161.2–193.3) at 1.5 min 171.3 (134.3–234.1) median all samples SOT/EDA 96.2 (82.6–123.0) baseline 121.4 (110.4–132.0) at 1.5 min 106.8 (96.7–157.1) median all samples No interventions 131.6 (97.1–227.2) basal 190.6 (121.0–234.6) at 1.5 min 144.1 (93.2–224.8) median all samples Important findings: Median all samples SOT/EDA significantly lower vs other groups (p = 0.033–0.005) with depressed profile, both basal and peak levels Higher SOT IV dose (in SOT IV and SOT/EDA groups) correlated with significantly lower median oxytocin (p = 0.019), mainly due to lower levels in SOT/EDA, see Fig. 3 |
Assay: ELISA ELISA gives higher levels than RIA with different effect patterns Comments: The combination of SOT and epidural gave rise to a unique depressed oxytocin effect pattern Other reported data: Oxytocin levels during breastfeeding at 2 days following labour epidural analgesia (This data to be reviewed in subsequent systematic reviewa) Blood pressure and personality changes in relation to SOT and other interventions (Data published elsewhere) Data from this study also published in Handlin et al. (2009) |
Postpartum: 13 women Postpartum SOT IM, no SOT in labour 20 women Spontaneous labour, no SOT or other interventions in labour or postpartum All women primiparous |
Dose regimens: SOT postpartum IM injection: 10 IU (8.3 μg)b Sampling regimen: During breastfeeding at 24–48 hr. postpartum with SSC Baseline at first latch then 15 samples at 30 sec intervals over first 7.5 min and at 10, 20, 30 and 60 min |
Results: Median (interquartile range), pg/mL With SOT IM postpartum 159.3 pg/mL(100.1–219.6) basal 173.0 (122.1–205.8) at 1.5 min 158.2 (119–187.2) median all samples No SOT 131.6 (97.1–227.2) basal 190.6 (121.0–234.6) at 1.5 min 144.1 (93.2–224.8) median all samples Important findings: Median levels in SOT IM group not significantly different to No SOT group, with similar pattern of oxytocin release in response to breastfeeding |
Assay: ELISA ELISA gives higher levels than RIA with different effect patterns Other reported data: Oxytocin levels during breastfeeding at 2 days following labour epidural analgesia (This data to be reviewed in subsequent systematic reviewa) Blood pressure and personality changes in relation to SOT and epidurals (Data published elsewhere) |
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Takahashi et. al. (2021) Epidural Analgesia With or Without Oxytocin, but Not Oxytocin Alone, Administered During Birth Disturbs Infant Pre-feeding and Sucking Behaviors and Maternal Oxytocin Levels in Connection With a Breastfeed Two Days Later [updated search 2022 Rev1] |
Intrapartum: 5 women Labour augmentation with SOT 10 women Labour augmentation with SOT plus EDA 13 women Spontaneous labour, no SOT or other interventions All women primiparous |
Dose regimens: SOT IV infusion: Total doses: Median 1.1 IU (1.86 μg) IQR 0.7–3.0 IU (1.145–5.046 μg) SOT IV infusion with epidural (SOT + EDA): Total dose: Median 2.5 IU (4.16 μg) IQR 0.89–3.78 IU (1.487–6.308 μg) Sampling regimen: (see Jonas above) |
Results: Group means±SE, pg/mL (Estimated from Fig. 2) Mean: mean of OT levels from 0 to 60 min Variance: mean of OT variance between 0 and 7.5 mins SOT/No EDA 190 ± 80 mean 830 ± 200 variance SOT + EDA 110 ± 30 mean 820 ± 100 variance No interventions 160 ± 55 mean 780 ± 130 variance Important findings: No significant difference in mean OT levels or variance in SOT group vs controls. Lowest mean OT in SOT + EDA group (p < 0.005 vs SOT, p < 0.005 vs controls) |
Assay: ELISA ELISA gives higher levels than RIA with different effect patterns Comments: Variance reflects pulsatility of oxytocin release Other reported data: Breastfeeding behaviour, IBFAT score: Shorter duration of rooting in: SOT vs controls (p < 0.05); SOT + EDA vs controls (p < 0.0001) and SOT vs SOT + EDA (p < 0.0001) Oxytocin levels during breastfeeding at 2 days following labour epidural analgesia (This data to be reviewed in subsequent systematic reviewa) Blood pressure, and personality changes in relation to SOT and other interventions (Data published elsewhere) Data from this study also published in Jonas et al. (2009) and Handlin et al. (2009) |
Postpartum: 8 women Postpartum SOT IM (no SOT in labour) 13 women Spontaneous labour, no SOT or other interventions in labour or postpartum All women primiparous |
Dose regimens: SOT postpartum IM injection: 10 IU Sampling regimen: (see Jonas above) |
Results: Group means±SE, pg/mL (Estimated from Fig. 2) Mean: mean of OT levels from 0 to 60 min Variance: mean of OT variance between 0 and 7.5 mins SOT IM postpartum 165 ± 50 mean 870 ± 200 variance No SOT (Controls) 160 ± 55 mean 780 ± 260 variance Important findings: No significant difference in mean OT levels or variance in SOT IM group vs. controls. |
Assay: ELISA ELISA gives higher levels than RIA with different effect patterns Comments: Variance reflects pulsatility of oxytocin release Other reported data: Breastfeeding behaviour, IBFAT score: Shorter duration of rooting in SOT IM vs controls (p < 0.0001) Oxytocin levels during breastfeeding at 2 days following labour epidural analgesia (This data to be reviewed in subsequent systematic reviewa) Blood pressure, cortisol levels and personality changes in relation to SOT and other interventions (Data published elsewhere) Data from this study also published in Jonas et al. (2009) and Handlin et al. (2009) |
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Administration of synthetic oxytocin with later postpartum sampling: combined exposed/unexposed analysis | ||||
Erickson et.al. (2020) Oxytocin, Vasopressin and Prolactin in New Breastfeeding Mothers: Relationship to Clinical Characteristics and Infant Weight Loss |
46 women Spontaneous labour With (11) and without (35) SOT augmentation in labour, birth 18/46 also received epidural analgesia 33/46 women also received postpartum SOT |
Dose regimen: Not stated Total or maximum dose: Intrapartum Max infusion rate: 20 mU/min Max duration: 12 hours Total intrapartum dose: mean 1.3 IU (SD 1.3) Postpartum Dose not stated Total SOT (intra and postpartum) Mean 8.9 IU (SD 8.3) Sampling regimen: 4–5 days postpartum (n = 35) Blood sampled at breastfeeding commencement and 20 min later (n = 32 with > = 1 successful samples) |
Results: (Oxytocin levels not given for women with SOT vs no SOT) Mean ± SD (all women) Basal 1641.5 ± 121.7 pg/mL baseline 20 mins breastfeeding 1713.6 ± 127.2 Important findings: Significantly higher basal levels in women with higher SOT dose in labour (p = 0.03) |
Assay: ELISA ELISA gives higher levels than RIA with different effect patterns Comments: Mixture of intra- and post-partum exposures Data used for correlations not provided Other reported data: Oxytocin in relation to birth and breastfeeding Significant increase in mean oxytocin (all women) at 20 min breastfeeding (p < 0.001) Higher basal oxytocin correlated with shorter labour (p = 0.003) AVP and prolactin during breastfeeding Women administered SOT in labour had increase in AVP levels from basal to 20 min breastfeeding, whereas women without SOT had reduced AVP (p = 0.03) |
Gu V. et.al. (2016) Intrapartum Synthetic Oxytocin and Its Effects on Maternal Well-Being at 2 Months Postpartum Data includes several study populations, including two groups of women (stated as n = 287) who appear to be included in Prevost (2014) |
386 women With and without SOT in labour, birth, postpartum 29/386 without SOT exposure included in combined analysis |
Dose regimen: Intrapartum 2 mU/min increasing by 2 mU/min to maximum 20 mU/min Postpartum Intramuscular injection, stated as “standard dose 100 μg converted to 50 IU” Total or maximum dose: Mean 36.61 IU (SD 24.36) including postpartum dosage Sampling regimen: Single blood sample at home visit at 2 months postpartum (n = 318) |
Results: (Oxytocin levels not given for women with SOT vs no SOT) Mean ± SD (all women) 281.02 ± 233.66 pg/mL Important findings: SOT total dose significantly predicted oxytocin levels at 2 months (p < 0.001) and accounted for 2.2% of the variance (data not provided) Women who were exclusively breastfeeding at 2 months postpartum had received significantly less SOT vs non-exclusively breastfeeding women (p < 0.001, data not provided) |
Assay: ELISA, not extracted ELISA gives higher levels than RIA with different effect patterns Comments: Study design combines several populations Numbers of women included and sampled appear contradictory Reported intramuscular postpartum dose is very high (50 IU) in comparison to other included studies and to standard clinical practice (5-10 IU) Total dose is very high in comparison to other included studies Other reported data: SOT and mental health Higher SOT dose associated with greater (self-reported) depressive, anxious, and somatization symptoms (p < 0.05), and accounted for 4.7% of variance in depression symptoms |
Prevost et.al. (2014) Oxytocin in pregnancy and the postpartum: relations to labor and its management. This study population appears to be also included in Gu (2016) |
272 women Some women had SOT for induction or augmentation (numbers not stated) |
Dose regimen: Not stated Total or maximum dose: (Calculated from data in Table 2) Total dose 0.58–3.02 IU Overall mean total dose: 1.4 IU Sampling regimen: Single blood sample at home visit at 2 months postpartum |
Results: (Oxytocin levels not given for women with SOT vs no SOT) Mean ± SD, pg/mL All women 286.3 ± 272.7 Important findings: SOT total dose positively associated with oxytocin levels (data and significance not provided) Each extra IU SOT in labour increased oxytocin levels by 15.6 pg/mL (95% CIs: 5.7, 25.5) |
Assay: ELISA, not extracted ELISA gives higher levels than RIA with different effect patterns Comments: Very high individual variability Study design combines two different populations Low doses unlikely to significantly raise oxytocin levels in labour No tests of significance given Other reported data: Oxytocin variability: Oxytocin (all samples, including during pregnancy) varied 70-fold between individuals (32.3–2297.6 pg/mL) Oxytocin and breastfeeding: Higher oxytocin levels (basal) in non-breastfeeding vs. breastfeeding women Oxytocin in pregnancy: Levels fell from early to late pregnancy in 73 women (27%) |
Units: IU international units, mU milliUnits, μU microunits, μg or mcg micrograms, ng nanograms, pg picograms, pmol picomoles, mL millilitres
Oxytocin conversions: 1 IU = 1000 mU; 1 mU = 1000 μU; 1 mg = 1000 μg; 1 μg = 1000 ng; 1 ng = 1000 pg; 1 IU = 1.67 μg; 1 mU = 1.67 ng; 1 μU = 1.67 pg; 1 μg = 0.6 IU; 1 ng = 0.60 mU; 1 pg/mL = 1 pmol/L = 1pM
Abbreviations: approx approximately, AVP arginine vasopressin, CI confidence intervals, cm centimetres of cervical dilation, EDA epidural analgesia, ELISA enzyme-linked immunoassay (EIA also used), fig figure, hr hour, IM intramuscular, IQR interquartile range, IV intravenous, MCR metabolic clearance rate, min minutes, PG prostaglandin, PGE2 prostaglandin E2, PGF2α prostaglandin F2alpha (13,14-dihydro-15-keto-prostaglandin F2 alpha), PGFM 13,14-dihydro-15-keto-PGF2α (PGF2alpha metabolite), RIA radioimmunoassay, ROM rupture of membranes, SD standard deviation, SEM standard error of the mean, sec seconds, SOT synthetic oxytocin, SSC skin-to-skin contact with newborn, UA umbilical artery, UV umbilical vein, vs versus, wk week
aFurther systematic reviews (manuscripts in preparation) will report maternal and newborn plasma oxytocin levels in relation to caesarean section, epidural analgesia, opioid analgesia, prostaglandins, ROM and other interventions
bSOT postpartum intramuscular dose incorrectly reported in publication as 8.3 μg (10 IU), when actual dose was 16.7 μg =10 IU, as verified with authors