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DOI: 10.1055/a-1538-2200
Labour Induction with Misoprostol in German Obstetric Clinics: What Are the Facts on Such Use?
Artikel in mehreren Sprachen: English | deutschAbstract
Subject While the synthetic prostaglandin E1 analogue misoprostol is the most effect labour induction agent, its use is off-label for the most part. For this reason, and in view of its potential adverse effects and varying approaches to its administration, the drug has recently once again become a focus of critical attention. The objective of this survey was thus to establish a record of labour induction with misoprostol in German clinics and determine the impact of the negative reporting on everyday obstetric practice.
Material and Methods In this cross-sectional study, 635 obstetrics and gynaecology departments in Germany were requested by email to participate in our survey in February/March 2020. Online responses to 19 questions were requested regarding the clinic, use of misoprostol before and after the critical reporting, use of misoprostol (sourcing, method of administration, dosage, monitoring) and other labour induction methods.
Results A total of 262 (41.3%) of the clinics solicited for the survey completed the questionnaire. There were no differences regarding the care level (Perinatal Centre Level I, Perinatal Centre Level II, Clinic with Perinatal Focus or Obstetric/Private Clinic; p = 0.2104) or birth counts (p = 0.1845). In most cases, misoprostol was prepared in the clinicʼs own pharmacy (54%) or imported from another country (46%) and administered orally in tablet form (95%). Misoprostol dosage levels varied (25 µg [48%], 50 µg [83%], 75 µg [6%], 100 µg [47%] and > 100 µg [5%]). Most of the clinics used premanufactured tablets/capsules (59%), although Cytotec tablets were also divided (35%) or dissolved in water (5%). Misoprostol administration intervals were mainly every 4 hours (64%) or every 6 hours (30%). CTG checks were run in most cases before and after administration of a dose of misoprostol (78% and 76%) and before and after administration of a dose of prostaglandin E2 (both 88%). Presence of contractions led to no misoprostol (59%) or no prostaglandin E2 (64%) being administered in most cases. The critical reporting resulted in discontinuation of use of misoprostol in 17% of the clinics – mainly smaller obstetric/private clinics with fewer than 1000 births. Labour cocktails were used mainly in obstetric and private clinics (61%).
Conclusion Misoprostol is an established agent for labour induction in German clinics. The dosing schemes used vary. Improvements of currently common management practices are required, especially in the area of labour induction (CTG checks before and after administration of labour-inducing medication, no administration of prostaglandin if contractions are ongoing). The discussion of use of misoprostol in the media resulted in stoppage of its use mainly in smaller clinics.
#
Introduction
The past 10 years have seen publication of nearly a dozen meta-analyses on use of misoprostol for labour induction and its efficacy and safety compared to oxytocin, dinoprostone and balloon catheters [1], [2], [3], [4], [5], [6], [7], [8], [9], [10]. Misoprostol can be administered both vaginally and orally and is considered the most effective labour induction agent in cases of immature cervix [2], [3]. Like all medicinal products (prostaglandin E2, oxytocin), misoprostol may also cause overstimulations resulting in changes in the CTG pattern. The risk of an overstimulation is increased in particular with vaginal administration and at higher dosage levels [3], [5], [11], [12]. Use of misoprostol for labour induction in women with prior caesarean sections is not recommended [13], [14], [15], [16]. The main reason for this is that the sole randomized, controlled study (comparison of vaginal misoprostol versus oxytocin) was prematurely discontinued following the occurrence of two uterus ruptures and recruitment of 17 patients [17]. There are also mainly retrospective studies in which misoprostol was administered only vaginally using various dosages and intervals [18], [19]. According to a Cochrane analysis, not a single uterus rupture occurred following oral administration of misoprostol in 158 pregnant women [20]. Notwithstanding the fact that misoprostol has now been authorized in various countries for labour induction, discussions of this theme arise repeatedly in German-speaking countries, where it is/was only authorized for prevention and treatment of gastroduodenal ulcers, but not for labour induction. Recent articles in the German press have discussed the legality of use of misoprostol for labour induction as a hot button issue with a focus on the lack of marketing authorization, lack of recommendations on dosage and use and potential associations with complications (e.g. overstimulations, pathological CTG, poor child outcomes) [21]. It is indeed not known how often misoprostol is used for labour induction in German clinics, with data also lacking on how the drug is prepared, administered and dosed. The last survey from 2013 revealed that many different regimens were in use [22].
The objective of this survey was thus to establish a record of labour induction with misoprostol in German clinics and determine the impact of the negative reporting on everyday obstetric practice.
#
Material and Methods
Participants and setting
In this cross-sectional study, invitations were extended to 635 obstetrics and gynaecology departments in Germany. The respective department heads were provided with a link to the questionnaire in an email together with a cover letter explaining the objective and design of the study. The questionnaire was developed based on national and international recommendations and guidelines. To ensure clarity and feasibility, the questionnaire was pre-tested by three experienced obstetricians who had not contributed to development of the survey. Modifications were made based on the resulting feedback. The results of these pre-tests were not taken into account in the final data evaluation. The final questionnaire comprised a total of 19 multiple choice and open questions covering the following topics:
-
Demographic aspects of the respective obstetric units (3 questions)
-
Use of misoprostol before and after current discussion (3 questions)
-
Misoprostol sourcing (1 question)
-
Misoprostol administration (6 questions)
-
Misoprostol dosage schemes (2 questions)
-
Clinic-specific labour induction management (1 question)
-
Clinic-specific labour induction alternatives (3 questions)
The survey was conducted pseudonymously. A maximum of two reminders were sent out 14 and 21 days after the first invitation to participate. No personal data were recorded.
#
Data collection
Data were collected from 24 February to 20 March 2020 on a voluntary basis with no remuneration of the participating clinics. An online survey format was chosen to facilitate Germany-wide participation. The participation link was available at www.soscisurvey.de (source: Stelzl P, Survey [Version 3.2.14i], https://www.soscisurvey.de, accessed 20 December 2020). This online platform ensured a high level of data protection because the IP addresses of the participating clinics were not recorded. Each participant was allowed to fill out the questionnaire just once during the 26-day survey period. To ensure complete responses, a warning message reminded participants to furnish missing responses before they could access the next page of the survey. A total of 262 of the 635 solicited clinics completed the questionnaire for a response rate of 41.3%. At the end of the survey period, the collected data were exported to an Excel table and forwarded for statistical analysis.
#
Statistical analysis
All statistical calculations and analyses were done with the statistics program package SAS, Release 9.4 (SAS Institute Inc., Cary, North Carolina, USA). Both absolute and relative frequencies are indicated for all responses to the multiple choice questions. To compare two or more groups, an χ2 test was used or (if the conditions for that test type were not met) a Fisherʼs exact test. The Mann-Whitney U test, or for more than two groups the Kruskal-Wallis test, was used for ordinal scale characteristics. Missing values or responses such as “donʼt know” were not considered for the analyses. A multiple logistic regression analysis was performed for each outcome to determine which combination of impact parameters (medical care level, births per year, labour induction rate) provided the best explanation for the respective outcome. Generally speaking, a test result was considered significant if the p value was below 0.05. A significance level of 0.10 was assumed for the multiple regression analyses to render the combined impact of multiple factors more recognizable.
#
#
Results
[Table 1] presents the demographic parameters of the clinics that either used or did not use misoprostol in Cytotec prior to the critical reporting. There was no statistically significant difference in use of misoprostol between the different care levels (Perinatal Centre Level I, Perinatal Centre Level II, Clinic with Perinatal Focus or Obstetric/Private Clinic; p = 0.2104). Use of the substance was also independent of the number of births (p = 0.1845). A trend towards significance was seen in the impact of the labour induction rate (p = 0.0518). It was observed that misoprostol was used particularly often in clinics with moderate labour induction rates of between 20 and 30%.
|
Misoprostol (n = 221, 84%) |
No misoprostol (n = 41, 16%) |
p values |
|
|---|---|---|---|
|
Perinatal Centre Level I |
76 (89%) |
9 (11%) |
0.2104 |
|
Perinatal Centre Level II |
20 (77%) |
6 (23%) |
|
|
Clinic with Perinatal Focus |
38 (78%) |
11 (22%) |
|
|
Obstetric/Private Clinic |
87 (85%) |
15 (15%) |
|
|
Births per year |
0.1845 |
||
|
16 (94%) |
1 (6%) |
|
|
72 (78%) |
20 (22%) |
|
|
49 (84%) |
9 (16%) |
|
|
42 (86%) |
7 (14%) |
|
|
27 (90%) |
3 (10%) |
|
|
15 (94%) |
1 (6%) |
|
|
Labour induction rate |
0.0518 |
||
|
69 (78%) |
20 (22%) |
|
|
143 (88%) |
19 (12%) |
|
|
9 (82%) |
2 (18%) |
Sourcing and method of administration of misoprostol
Sourcing and administration of misoprostol varied in the different clinics as shown in [Table 2]. Misoprostol was prepared in the clinic pharmacy in about half of the cases (54%) or imported from other countries (46%). These figures did not differ amongst the different care levels (p = 0.8185). Sourcing of the agent did not correlate with either number of births per year or labour induction rate (p = 0.8398/p = 0.8795, [Tables 8] and [9]).
|
Total (n = 221) |
PNC Level I (n = 76) |
PNC Level II (n = 20) |
Clinic with Perinatal Focus (n = 38) |
Obstetric/Private Clinic (n = 87) |
p values |
|
|---|---|---|---|---|---|---|
|
* Multiple responses possible, ** Comparison of 50 µg initial dose versus other dose |
||||||
|
What was your source for misoprostol? |
||||||
|
Preparation in clinic pharmacy |
111 (54%) |
41 (56%) |
11 (58%) |
17 (47%) |
42 (53%) |
0.8185 |
|
Import from other country |
96 (46%) |
32 (44%) |
8 (42%) |
19 (53%) |
37 (47%) |
|
|
What method(s) of administration did you use?* |
||||||
|
Oral (tablet) |
209 (95%) |
73 (96%) |
20 (100%) |
35 (92%) |
81 (93%) |
0.5806 |
|
Oral (liquid) |
11 (5%) |
3 (4%) |
1 (5%) |
2 (5%) |
5 (6%) |
0.9664 |
|
Vaginal (tablet) |
56 (25%) |
22 (29%) |
3 (15%) |
9 (24%) |
22 (25%) |
0.6351 |
|
Vaginal (insert) |
26 (12%) |
13 (17%) |
2 (10%) |
4 (11%) |
7 (8%) |
0.3660 |
|
What dosage levels were used?* |
||||||
|
25 µg |
106 (48%) |
45 (59%) |
12 (60%) |
12 (32%) |
37 (43%) |
0.0175 |
|
50 µg |
183 (83%) |
67 (88%) |
13 (65%) |
33 (87%) |
70 (80%) |
0.0802 |
|
75 µg |
14 (6%) |
7 (9%) |
0 |
1 (3%) |
6 (7%) |
0.4763 |
|
100 µg |
104 (47%) |
38 (50%) |
4 (20%) |
14 (37%) |
48 (55%) |
0.0183 |
|
> 100 µg |
11 (5%) |
5 (7%) |
2 (10%) |
2 (5%) |
2 (2%) |
0.2966 |
|
Were dosage levels of 50 µg and more in general use? |
||||||
|
Yes |
196 (89%) |
70 (92%) |
15 (75%) |
34 (89%) |
77 (89%) |
0.2192 |
|
No |
25 (11%) |
6 (8%) |
5 (25%) |
4 (11%) |
10 (11%) |
|
|
How did you obtain the desired dosage form? |
||||||
|
Capsule/tablet dosed accordingly |
129 (59%) |
46 (61%) |
15 (75%) |
20 (53%) |
48 (57%) |
0.7987 |
|
Division of tablet |
77 (35%) |
25 (33%) |
5 (25%) |
16 (42%) |
31 (37%) |
|
|
Dissolution of tablet plus liquid in appropriate amount |
11 (5%) |
4 (5%) |
0 |
2 (5%) |
5 (6%) |
|
|
Other |
0 |
0 |
0 |
0 |
0 |
|
|
What dosing intervals were used for misoprostol?* |
||||||
|
Every 2 hours |
16 (7%) |
3 (4%) |
5 (25%) |
2 (5%) |
6 (7%) |
0.0316 |
|
Every 4 hours |
139 (64%) |
50 (66%) |
6 (30%) |
26 (68%) |
57 (66%) |
0.0113 |
|
Every 6 hours |
66 (30%) |
26 (34%) |
7 (35%) |
10 (26%) |
23 (26%) |
0.7124 |
|
Other |
8 (4%) |
1 (1%) |
2 (10%) |
0 |
5 (6%) |
0.1064 |
|
How many doses of misoprostol were administered per patient and day? |
||||||
|
One |
2 (1%) |
0 |
1 (5%) |
0 |
1 (1%) |
0.4921 |
|
Two |
27 (12%) |
7 (9%) |
3 (15%) |
8 (22%) |
9 (11%) |
|
|
Three |
107 (49%) |
37 (49%) |
9 (45%) |
17 (46%) |
44 (52%) |
|
|
Four |
65 (30%) |
26 (34%) |
4 (20%) |
10 (27%) |
25 (29%) |
|
|
Five |
6 (3%) |
3 (4%) |
0 |
1 (3%) |
2 (2%) |
|
|
Six |
8 (4%) |
2 (3%) |
2 (10%) |
1 (3%) |
3 (4%) |
|
|
More than six |
3 (1%) |
1 (1%) |
1 (5%) |
0 |
1 (1%) |
|
|
On how many successive days was (only) misoprostol used for labour induction? |
||||||
|
1 day |
11 (5%) |
3 (4%) |
1 (5%) |
2 (5%) |
5 (6%) |
0.0078 |
|
2 days |
103 (47%) |
26 (34%) |
11 (55%) |
23 (62%) |
43 (51%) |
|
|
3 days |
84 (39%) |
34 (45%) |
8 (40%) |
9 (24%) |
33 (39%) |
|
|
> 3 days |
20 (9%) |
13 (17%) |
0 |
3 (8%) |
4 (5%) |
|
|
What is the substance amount for the initial dose? |
||||||
|
25 µg |
90 (45%) |
36 (51%) |
11 (61%) |
12 (35%) |
31 (39%) |
0.1129** |
|
50 µg |
110 (55%) |
33 (47%) |
7 (39%) |
22 (63%) |
48 (61%) |
|
|
100 µg |
1 (0.5%) |
1 (1%) |
0 |
0 |
0 |
|
|
Use of dosage levels of 50 µg and more |
Pharmacy preparation |
Initial dose 50 µg |
No misoprostol after reporting |
No CTG check before or after prostaglandin dose |
Use of castor oil |
|
|---|---|---|---|---|---|---|
|
Clinics, total |
196 (89%) |
111 (54%) |
110 (55%) |
35 (17%) |
35 (14%) |
114 (46%) |
|
Births per year: |
||||||
|
< 500 |
15 (94%) |
8 (57%) |
6 (46%) |
8 (57%) |
3 (20%) |
8 (53%) |
|
500 – 999 |
64 (89%) |
37 (55%) |
41 (61%) |
9 (69%) |
11 (13%) |
55 (63%) |
|
1000 – 1499 |
43 (88%) |
20 (45%) |
25 (53%) |
7 (15%) |
9 (14%) |
23 (41%) |
|
1500 – 1999 |
35 (83%) |
25 (61%) |
18 (49%) |
6 (15%) |
7 (15%) |
12 (26%) |
|
2000 – 3000 |
25 (93%) |
15 (56%) |
10 (43%) |
4 (15%) |
3 (11%) |
10 (36%) |
|
> 3000 |
14 (93%) |
6 (43%) |
10 (71%) |
1 (7%) |
3 (19%) |
6 (38%) |
|
p value |
0.8900 |
0.8398 |
0.6025 |
0.0537 |
0.9677 |
0.0002 |
|
Use of dosage levels of 50 µg and more |
Pharmacy preparation |
Initial dose 50 µg |
No misoprostol after reporting |
No CTG check before or after prostaglandin dose |
Use of castor oil |
|
|---|---|---|---|---|---|---|
|
Total |
196 (89%) |
111 (54%) |
110 (55%) |
35 (17%) |
35 (14%) |
114 (46%) |
|
Rate: |
||||||
|
< 20% |
62 (90%) |
35 (55%) |
39 (62%) |
14 (21%) |
10 (12%) |
48 (57%) |
|
20 – 30% |
125 (87%) |
71 (53%) |
64 (50%) |
20 (15%) |
24 (16%) |
63 (41%) |
|
> 30% |
9 (100%) |
5 (56%) |
8 (78%) |
1 (11%) |
1 (10%) |
3 (30%) |
|
p value |
0.8900 |
0.8795 |
0.3992 |
0.2388 |
0.5527 |
0.0117 |
Misoprostol was administered orally in tablet form in nearly all clinics (95%) ([Table 2]). It was additionally administered vaginally in tablet form in one clinic in four (25%), and more rarely in the form of inserts (12%). Administration of misoprostol dissolved in liquid for drinking was practised in only a few clinics (5%).
#
Dosage of misoprostol
Dosage of misoprostol varied in the different clinics. Generally speaking, dosage levels of 50 µg and above were used in most clinics (89%) independent of medical care level (p = 0.2192). Misoprostol dosage levels of 25 µg (48%), 50 µg (83%), 75 µg (6%), 100 µg (47%) and > 100 µg (5%) were used, whereby low doses of 25 µg were administered mainly in perinatal centres and higher doses of 100 µg were administered with notable frequency in obstetric clinics (p = 0.0175/p = 0.0183). In most clinics, the dosage forms were delivered prefabricated as tablets/capsules (58%). In the other cases, the Cytotec tablet was divided (35%) or dissolved in water (5%).
In most cases, misoprostol was administered every four hours (63%) or every six hours (30%), more rarely every two hours (7%) or at other intervals (4%). In Level 2 Perinatal Centres, misoprostol was administered more frequently, i.e. every two hours or, more rarely, every four hours (p = 0.0316/p = 0.0113). Depending on the dosage interval used, in most cases three (49%), four (30%) or two (12%) doses were administered per day. Use of misoprostol only was reported for two (47%) or three (39%) successive days, rarely for more than three days (9%) or for only one day (5%).
An initial dose of 50 µg (55%) or 25 µg (45%) was selected in nearly all clinics. The initial dose was 100 µg in one clinic only. The decision by a given clinic to begin with a dose of at least 50 µg was found to be independent of the respective medical care level (p = 0.1129); number of births and rate of labour inductions also did not influence this decision (p = 0.6025/p = 0.3922, [Tables 8] and [9]).
#
Impact of media reporting on use of misoprostol
[Table 3] shows the impact of the critical reporting on use of misoprostol. Use of misoprostol was discontinued in 17% of the clinics. This was independent of medical care level (p = 0.9436) and labour induction rate (p = 0.2388, [Table 9]). It was, however, observed that a high percentage (about 60%) of clinics with fewer than 1000 births per year discontinued use of misoprostol following the reporting (p = 0.0537, [Table 8]). The main reasons for this were worry about patient reactions, avoidance of having to justify decisions and fear of legal consequences (40% in each of these categories). In 31% of the clinics, further use was disallowed by the boss or clinic management. Changes were also instituted in the clinics that continued using misoprostol: Increased efforts to provide information characterized the main change (80% of cases), with only a few cases of a different induction scheme (6%) or a lower initial dose for induction (4%) being introduced.
|
Total (n = 211) |
PNC Level I (n = 73) |
PNC Level II (n = 20) |
Clinic with Perinatal Focus (n = 35) |
Obstetric/ |
p values |
|
|---|---|---|---|---|---|---|
|
* Multiple responses possible |
||||||
|
Is use of misoprostol continuing subsequent to the critical reporting? |
||||||
|
Yes |
176 (83%) |
61 (84%) |
17 (85%) |
28 (80%) |
70 (84%) |
0.9436 |
|
No |
35 (17%) |
12 (16%) |
3 (15%) |
7 (20%) |
13 (16%) |
|
|
What has changed? |
||||||
|
We have discontinued its use (n = 35), …* |
(n = 12) |
(n = 3) |
(n = 7) |
(n = 13) |
||
|
… because it was disallowed (boss/clinic management/…) |
11 (31%) |
4 (33%) |
2 (67%) |
1 (14%) |
4 (31%) |
0.4963 |
|
… because we fear legal consequences |
14 (40%) |
2 (17%) |
1 (33%) |
4 (57%) |
7 (54%) |
0.1936 |
|
… to avoid having to justify decisions to patients, due to worry about patient reactions, |
14 (40%) |
7 (58%) |
1 (33%) |
3 (43%) |
3 (23%) |
0.3404 |
|
We have continued its use (n = 176) …* |
(n = 61) |
(n = 17) |
(n = 28) |
(n = 70) |
||
|
… in lower single doses |
7 (4%) |
1 (2%) |
1 (6%) |
1 (4%) |
4 (6%) |
0.5116 |
|
… with a different treatment scheme (lower total dose) |
10 (6%) |
4 (7%) |
1 (6%) |
2 (7%) |
3 (4%) |
0.8932 |
|
… as before, but we must increase efforts to provide information |
141 (80%) |
51 (84%) |
12 (71%) |
23 (82%) |
55 (9%) |
0.6566 |
|
Other |
39 (22%) |
12 (20%) |
5 (29%) |
5 (18%) |
17 (24%) |
0.7479 |
#
Management for labour induction
Management of misoprostol use for labour induction is presented in [Table 4]. Written information was provided regarding the off-label use of misoprostol in 81% of cases. In cases of labour induction post prior caesarean section – regardless of the method used – written information was provided in only 24% of the clinics. Labour induction is an inpatient procedure in almost all such cases (97%). Medical labour induction is almost always carried out accompanied by CTG checks: This was done in 78% and 88% of the participating clinics before administration of misoprostol and prostaglandin E2 respectively. CTG checks were performed just as frequently after administration of a dose of misoprostol (76%) and prostaglandin E2 (88%). Cases in which no CTG check was performed before or after administration of a dose of prostaglandin showed no dependence on medical care level, number of births or labour induction rate (p = 0.8414, p = 0.9677, p = 0.5527). No misoprostol was administered in the presence of contractions in 146 clinics (59%). 159 clinics (64%) also administered no prostaglandin E2 if labour contractions were present.
|
Total (n = 249) |
PNC Level I (n = 81) |
PNC Level II (n = 26) |
Clinic with Perinatal Focus (n = 44) |
Obstetric/ |
p values |
|
|---|---|---|---|---|---|---|
|
Provision of written information on off-label use when misoprostol is used |
202 (81%) |
73 |
18 |
31 |
80 |
0.0188 |
|
Provision of written information on off-label use when labour is induced post prior caesarean section (condition post sectio) |
60 (24%) |
26 |
8 |
9 |
17 |
0.1010 |
|
Outpatient labour induction with misoprostol possible |
8 (3%) |
2 |
1 |
2 |
3 |
0.8347 |
|
CTG check before misoprostol dose |
193 (78%) |
69 |
16 |
29 |
79 |
0.0149 |
|
CTG check before prostaglandin E2 dose |
218 (88%) |
70 |
23 |
40 |
85 |
0.8895 |
|
CTG check after misoprostol dose |
189 (76%) |
68 |
15 |
30 |
76 |
0.0272 |
|
CTG check after prostaglandin E2 dose |
218 (88%) |
70 |
23 |
41 |
84 |
0.6374 |
|
No CTG check before or after prostaglandin dose |
35 (14%) |
11 |
3 |
5 |
16 |
0.8414 |
|
No misoprostol dose in the presence of contractions |
146 (59%) |
51 |
14 |
27 |
54 |
0.6798 |
|
No prostaglandin E2 dose in the presence of labour contractions |
159 (64%) |
51 |
16 |
31 |
61 |
0.7943 |
|
Raising of oxytocin dose every 10 – 20 minutes |
74 (30%) |
19 |
7 |
12 |
36 |
0.2557 |
|
Raising of oxytocin dose every 30 – 60 minutes |
102 (41%) |
39 |
10 |
15 |
38 |
0.4154 |
|
Raising of oxytocin dose at intervals > 60 minutes |
15 (6%) |
5 |
5 |
2 |
3 |
0.8676 |
|
Raising of oxytocin dose until contractions occur at 2 – 3 minute intervals |
22 (9%) |
9 |
1 |
3 |
9 |
0.7609 |
|
Raising of oxytocin dose until contractions occur at 4 – 5 minute intervals |
48 (19%) |
16 |
7 |
13 |
12 |
0.0693 |
|
Discontinuation of oxytocin administration for labour induction after 5 hours |
78 (31%) |
23 |
10 |
10 |
35 |
0.3437 |
|
Discontinuation of oxytocin administration for labour induction after 5 – 10 hours |
36 (14%) |
11 |
3 |
10 |
12 |
0.3839 |
|
Discontinuation of oxytocin administration for labour induction after 10 – 15 hours |
4 (2%) |
0 |
1 |
2 |
1 |
0.1100 |
|
Discontinuation of oxytocin administration for labour induction based only on clinical indication and CTG |
82 (33%) |
31 |
4 |
17 |
30 |
0.1353 |
|
Castor oil (outpatient or inpatient) |
114 (46%) |
25 |
11 |
18 |
60 |
0.0006 |
Differences between the clinics were seen in particular regarding the use of labour cocktails (outpatient or inpatient) (p = 0.0006): Their administration is comparatively frequent (61%) in obstetric clinics.
#
Alternative methods of labour induction
Alternative methods of labour induction in cases of immature cervix (Bishop Score < 3) are presented in [Table 5]. Frequent inpatient approaches in this situation are prostaglandin E2 (vaginal 84%, or cervical 56%) and balloon catheter (53%). Balloon catheters are used most frequently in Level I Perinatal Centres (77%) and infrequently in Clinics with Perinatal Focus (34%, p < 0.0001). Further options include dilapan (38%), labour cocktail (35%) and even oxytocin (29%). Outpatient management covering a variety of methods is only rarely offered (in fewer than 10% of the clinics).
|
Total (n = 249) |
PNC Level I (n = 81) |
PNC Level II (n = 26) |
Clinic with Perinatal Focus (n = 44) |
Obstetric/ |
p values |
|
|---|---|---|---|---|---|---|
|
* Multiple responses possible |
||||||
|
Dilapan (outpatient) |
19 (8%) |
5 |
4 |
1 |
9 |
0.1975 |
|
Dilapan (inpatient) |
94 (38%) |
28 |
11 |
20 |
35 |
0.6013 |
|
Balloon catheter (outpatient) |
9 (4%) |
3 |
2 |
1 |
3 |
0.6628 |
|
Balloon catheter (inpatient) |
133 (53%) |
62 |
14 |
15 |
42 |
< 0.0001 |
|
Prostaglandin E2/dinoprostone (gel, tablet, insert) (outpatient) |
4 (2%) |
2 |
0 |
1 |
1 |
0.7931 |
|
Prostaglandin E2/dinoprostone (gel, tablet, insert) (inpatient) |
208 (84%) |
66 |
20 |
39 |
83 |
0.5718 |
|
Prostaglandin E2/dinoprostone (cervical gel) (outpatient) |
4 (2%) |
2 |
0 |
1 |
1 |
0.7931 |
|
Prostaglandin E2/dinoprostone (cervical gel) (inpatient) |
140 (56%) |
46 |
16 |
23 |
55 |
0.8991 |
|
Oxytocin |
72 (29%) |
23 |
7 |
9 |
33 |
0.4449 |
|
Castor oil (outpatient) |
12 (5%) |
5 |
0 |
1 |
6 |
0.5788 |
|
Castor oil (inpatient) |
87 (35%) |
16 |
10 |
12 |
49 |
0.0002 |
|
Other |
15 (6%) |
3 |
4 |
1 |
7 |
0.1340 |
Oxytocin (85%), vaginal prostaglandin E2 (73%) and labour cocktail (39%) are most frequently selected for induction when the cervix is mature ([Table 6]). Approaches using cervical prostaglandin E2 (31%), balloon catheter (24%) and dilapan (8%) are also used. Labour cocktails in cases of mature cervix are administered more frequently in obstetric clinics (p = 0.0431).
|
Total (n = 249) |
PNC Level I (n = 81) |
PNC Level II (n = 26) |
Clinic with Perinatal Focus (n = 44) |
Obstetric/ |
p values |
|
|---|---|---|---|---|---|---|
|
Dilapan (outpatient) |
3 (1%) |
1 |
1 |
0 |
1 |
0.5040 |
|
Dilapan (inpatient) |
21 (8%) |
5 |
3 |
6 |
7 |
0.4339 |
|
Balloon catheter (outpatient) |
5 (2%) |
1 |
2 |
0 |
2 |
0.2142 |
|
Balloon catheter (inpatient) |
59 (24%) |
25 |
4 |
7 |
23 |
0.1891 |
|
Prostaglandin E2/dinoprostone (gel, tablet, insert) (outpatient) |
6 (2%) |
1 |
0 |
2 |
3 |
0.5629 |
|
Prostaglandin E2/dinoprostone (gel, tablet, insert) (inpatient) |
181 (73%) |
60 |
22 |
28 |
71 |
0.2885 |
|
Prostaglandin E2/dinoprostone (cervical gel) (outpatient) |
1 (0.4%) |
0 |
0 |
0 |
1 |
1.0000 |
|
Prostaglandin E2/dinoprostone (cervical gel) (inpatient) |
77 (31%) |
24 |
6 |
9 |
38 |
0.1166 |
|
Oxytocin |
211 (85%) |
69 |
24 |
38 |
80 |
0.5755 |
|
Castor oil (outpatient) |
11 (4%) |
2 |
0 |
2 |
7 |
0.3920 |
|
Castor oil (inpatient) |
97 (39%) |
23 |
9 |
17 |
48 |
0.0431 |
|
Other |
16 (6%) |
3 |
2 |
2 |
9 |
0.4753 |
#
Labour induction in condition post sectio
If a patient history includes a caesarean section, the favoured approaches to induction are oxytocin (63%) and vaginal prostaglandin E2 (61%) as well as the mechanical methods, balloon catheter (49%, especially at Level I Perinatal Centres at 73%) and dilapan (35%) ([Table 7]). Only 2% of the clinics generally eschew labour induction in condition post sectio.
|
Total (n = 243) |
PNC Level I (n = 81) |
PNC Level II (n = 26) |
Clinic with Perinatal Focus (n = 42) |
Obstetric/ |
p values |
|
|---|---|---|---|---|---|---|
|
Dilapan (outpatient) |
6 (2%) |
1 |
0 |
1 |
4 |
0.6422 |
|
Dilapan (inpatient) |
86 (35%) |
25 |
13 |
16 |
32 |
0.3391 |
|
Balloon catheter (outpatient) |
7 (3%) |
2 |
1 |
1 |
3 |
0.9472 |
|
Balloon catheter (inpatient) |
118 (49%) |
59 |
12 |
14 |
33 |
< 0.0001 |
|
Prostaglandin E2/dinoprostone (gel, tablet, insert) (outpatient) |
4 (2%) |
1 |
0 |
1 |
2 |
1.0000 |
|
Prostaglandin E2/dinoprostone (gel, tablet, insert) (inpatient) |
149 (61%) |
48 |
21 |
23 |
57 |
0.1666 |
|
Prostaglandin E2/dinoprostone (cervical gel) (outpatient) |
2 (1%) |
1 |
0 |
0 |
1 |
1.0000 |
|
Prostaglandin E2/dinoprostone (cervical gel) (inpatient) |
65 (27%) |
23 |
6 |
8 |
28 |
0.5713 |
|
Oxytocin |
152 (63%) |
49 |
18 |
27 |
58 |
0.8674 |
|
Castor oil (outpatient) |
3 (1%) |
0 |
1 |
1 |
1 |
0.2618 |
|
Castor oil (inpatient) |
77 (32%) |
19 |
8 |
12 |
38 |
0.1092 |
|
Other |
24 (10%) |
8 |
1 |
6 |
9 |
0.6060 |
Generation of a multiple statistical model using logistic regression analysis was only feasible for the outcome “Use of labour cocktail”, whereby the significance level was set at 0.10. The observation was made that annual birth count (p < 0.0001) and medical care level (p = 0.0893) impact this parameter independently. For the other parameters (initial dose 50 µg, use of dosages of 50 µg and more, no misoprostol after reporting) a multiple analysis revealed that only a single parameter was significant in each case (whereby the significance level was set at α = 0.10).
#
#
Discussion
41% of the 635 clinics solicited for this national survey, which represented different obstetric care levels, completed the questionnaire. It can be assumed that this study provides a representative overview of labour induction as practised in Germany. Misoprostol was used for labour induction in most of the clinics when the survey was conducted. This was true regardless of care level and clinic size. This confirms that misoprostol represents a standard method of medical labour induction.
A survey in 2013 revealed that a majority of clinics (66%) were already using misoprostol for labour induction at that time [22].
In most cases, misoprostol was prepared in the clinicʼs own pharmacy (54%) or imported from another country (45%) and administered orally in tablet form (95%). It was also administered vaginally in tablet form in one of four clinics (25%) and in some clinics in the form of inserts (12%). However, the misoprostol insert which has marketing authorization is now no longer available.
The desired dosage was ensured with prefabricated tablets/capsules (59%). The Cytotec tablet (200 µg) was divided (35%) or dissolved in water (5%) in the remaining cases. This manual division of the Cytotec tablets is an ill-advised procedure now condemned as such by both the current guideline recommendations and a “Red Hand Letter” issued by the Federal Institute for Drugs and Medical Devices (Bundesinstitut für Arzneimittel und Medizinprodukte – BfArM) [13], [15], [16], [23]. Despite the WHO recommendation, dissolving the tablet in water should also not be done due to the resulting imprecision as to stability and active pharmaceutical ingredient concentration [24].
There are no uniform recommendations for misoprostol dosage. 25 µg doses are recommended internationally and it is reported that lower dosage levels (up to 50 µg) are associated with outcomes similar to those obtained with higher dosages (100 µg) [24]. A further decisive factor in addition to dosage is the route of administration: A very large meta-analysis (611 studies, 31 different methods) confirmed that vaginal misoprostol in a dosage of ≥ 50 µg resulted in more cases of overstimulation than placebo (OR 4.40, 95% CI 2.22 – 7.94), but revealed no differences in the rate of transfers to paediatric clinics (OR 0.85, 95% CI 0.57 – 1.23) [11]. Similar data resulted for oral administration of misoprostol in a dosage of ≥ 50 µg per tablet (OR 2.85, 95% CI 1.41 – 5.20 and OR 0.83, 95% CI 0.55 – 1.20). The Swiss Association of Gynaecology and Obstetrics (Schweizerische Gesellschaft für Gynäkologie und Geburtshilfe), in their Expert Brief No. 63 from 2019, recommend dosage levels of 25 – 50 µg vaginally and 20 – 50 µg orally [13]. The S2k Induction of Labour Guideline describes single doses of 25 – 100 µg as possible [15], [16]. An oral misoprostol preparation slated to become available in Germany this year has received marketing authorization for single doses up to 50 µg and a maximum daily dose of 200 µg. This preparation is already available in Austria [25]. The survey from 2013 revealed that many different regimens were in use [22]. Studies on labour induction with misoprostol in German clinics also revealed a variety of treatment schemes [26], [27], [28]. This diversity has remained unchanged: According to the current survey, the misoprostol dosages most frequently used were 25 µg (48%), 50 µg (83%) and 100 µg (47%). Dosages > 100 µg (5%) were the exception and should be avoided according to current recommendations. The initial dose in nearly all treatment schemes was 50 µg or 25 µg. The interval between doses was in most cases 4 hours (64%) or 6 hours (30%), resulting in most cases in three (49%), four (30%) or two daily doses (12%). Use of the different dosages or intervals was determined to be independent of medical care level.
Misoprostol use in this context was off-label when the survey was carried out, making provision of appropriate information obligatory. This information was provided in written form as well in 81% of cases. Provision of such information in written form is generally recommended in cases of off-label use [13], [15], [16].
Induction of labour with misoprostol was almost always done in an inpatient setting (97%). Despite this being practised in outpatient settings as well internationally [29] this is discouraged in current recommendations. Medical labour induction should be performed in an inpatient setting under CTG control [13], [15], [16].
Earlier guidelines, now out of date, recommended dosing of prostaglandins accompanied by CTG checks and not using prostaglandins in the presence of contractions [30]. However, a pre-dosing CTG check was performed in only 78% of the clinics surveyed when misoprostol was administered and in 88% when prostaglandin E2 was used. Percentages of CTG checks after dosing of misoprostol and prostaglandin E2 were similar (76% and 88%). Also, misoprostol was administered despite the presence of contractions in 41% of the clinics, which figure was 36% for prostaglandin E2. This practice must be viewed critically, since prostaglandins can cause overstimulations. CTG checks before and after dosing of prostaglandins, and doing without prostaglandins in the presence of contractions, thus raise the safety level of this medical labour induction practice and should be done [15], [16]. It turns out that complications associated with misoprostol, and with prostaglandins in general, are not a matter of dosage, but rather of medical labour induction management in the broader sense. This certainly underscores the importance of the information provided in the new S2k Guideline regarding these points.
Labour induction in condition post sectio is associated with a raised risk of uterus rupture, even though the absolute risk level is low. Accordingly, both earlier and current labour induction guidelines characterize labour induction post sectio caesarea as a possible option [15], [16], [31], [32]. In the current survey, nearly all clinics reported performing labour induction in this situation (98%). However, information in written form regarding off-label use with the available methods is provided in only 24%. This aspect could become legally relevant, for which reason provision of this information in written form is recommended [15], [16].
The critical reporting on Cytotec led to discontinuation of use of misoprostol for labour induction in 17% of the clinics. The main reasons for this were worry about patient reactions, avoidance of having to justify decisions and fear of legal consequences (40% in each of these categories). In many cases (31%) further use was disallowed by the boss or clinic management. This is an impressive demonstration of the power of the press to impact obstetric medical care. In smaller clinics in particular, which depend on every single birth, discontinuation of the drug for this indication was observed above all in clinics with fewer than 500 births, but the critical reporting resulted only in increased efforts to provide information accordingly in other clinics (80%). There were only a small number of cases of shifts to other induction treatment schemes (6%) or reduction of individual doses (4%).
This situation should be viewed critically, since one of the alternative methods of labour induction was listed as the labour cocktail. The labour cocktail, for its part, is uniquely guilty of the aspects criticized in the press: It has no marketing authorization and evidence of safety and efficacy are lacking – this despite its use for labour induction over nearly a century [33], [34]. The benefit of this method is not evidence-based [35] and adverse effects/complications are known [36]. The labour cocktail is therefore not recommended for labour induction in international guidelines [37]. This is a plausible consequence in view of the fact that the active pharmaceutical ingredient, ricinoleic acid, achieves its effect on muscle cells in the uterus and intestine via prostaglandin receptors, so that the same potential adverse effects expected with use of misoprostol and prostaglandin E2 apply to it as well. Ricinus oil (castor oil) is therefore only suitable for labour induction in an inpatient setting and within the context of studies [15], [16].
Since the labour cocktail is used above all in smaller clinics (Obstetric/Private Clinic, p = 0.0006) with fewer than 1000 births per year and with lower labour induction rates (< 20%, p = 0.0117), the worry is justified that precisely those clinics that decide to discontinue use of misoprostol because of the critical reporting will increasingly turn to use of the labour cocktail [38]. This represents a sacrifice of quality in medical labour induction and puts patients and children at greater risk.
In summary, this survey provides a good current overview of labour induction as practised in German clinics. Other surveys are in some cases dated (from 2013 [22]) or were intended primarily for midwives [38]. Since this study did not aim to determine complication rates, future studies should analyse the spectrum of adverse effects/complications associated with a labour induction, in particular when misoprostol is administered.
#
Conclusion
This study demonstrates impressively that misoprostol, and use of prostaglandins generally speaking, represents an established method in Germany. It also points up the need for further improvement of certain procedures (e.g. dosage of misoprostol, monitoring). These imperatives have been known for some time, for which reason development of the S2k Induction of Labour Guideline was initiated, leading to its publication in December 2020. The Guideline will contribute to improvements in the labour induction procedure. Some of the criticism expressed in the media may be justified, but the way it was presented is itself deserving of criticism. It was revealed that the reporting resulted in discontinuation of use of misoprostol mainly in smaller clinics, giving rise to the concern that poorly investigated methods such as administration of ricinus oil (castor oil) will take its place. This would represent a sacrifice of quality in medical labour induction and put patients and children at greater risk.
#
#
Conflict of Interest/Interessenkonflikt
The authors declare that they have no conflict of interest./Die Autorinnen/Autoren geben an, dass kein Interessenkonflikt besteht.
-
References/Literatur
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Correspondence/Korrespondenzadresse
Publikationsverlauf
Eingereicht: 07. April 2021
Angenommen nach Revision: 25. Juni 2021
Artikel online veröffentlicht:
09. August 2021
© 2021. The Author(s). This is an open access article published by Thieme under the terms of the Creative Commons Attribution-NonDerivative-NonCommercial License, permitting copying and reproduction so long as the original work is given appropriate credit. Contents may not be used for commecial purposes, or adapted, remixed, transformed or built upon. (https://creativecommons.org/licenses/by-nc-nd/4.0/)
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-
References/Literatur
- 1 Ornat L, Alonso-Ventura V, Bueno-Notivol J. et al. Health Outcomes and Systematic Analyses (HOUSSAY) Research Group. Misoprostol combined with cervical single or double balloon catheters versus misoprostol alone for labor induction of singleton pregnancies: a meta-analysis of randomized trials. J Matern Fetal Neonatal Med 2020; 33: 3453-3468
- 2 Alfirevic Z, Keeney E, Dowswell T. et al. Methods to induce labour: a systematic review, network meta-analysis and cost-effectiveness analysis. BJOG 2016; 123: 1462-1470
- 3 Chen W, Xue J, Peprah MK. et al. A systematic review and network meta-analysis comparing the use of Foley catheters, misoprostol, and dinoprostone for cervical ripening in the induction of labour. BJOG 2016; 123: 346-354
- 4 Chen W, Xue J, Gaudet L. et al. Meta-analysis of Foley catheter plus misoprostol versus misoprostol alone for cervical ripening. Int J Gynaecol Obstet 2015; 129: 193-198
- 5 McMaster K, Sanchez-Ramos L, Kaunitz A. Balancing the efficacy and safety of misoprostol: a meta-analysis comparing 25 versus 50 micrograms of intravaginal misoprostol for the induction of labour. BJOG 2015; 122: 468-476
- 6 Liu A, Lv J, Hu Y. et al. Efficacy and safety of intravaginal misoprostol versus intracervical dinoprostone for labor induction at term: a systematic review and meta-analysis. J Obstet Gynaecol Res 2014; 40: 897-906
- 7 Fox NS, Saltzman DH, Roman AS. et al. Intravaginal misoprostol versus Foley catheter for labour induction: a meta-analysis. BJOG 2011; 118: 647-654
- 8 Hofmeyr GJ, Gülmezoglu AM, Pileggi C. Vaginal misoprostol for cervical ripening and induction of labour. Cochrane Database Syst Rev 2010; 2010 (10) CD000941
- 9 Austin SC, Sanchez-Ramos L, Adair CD. Labor induction with intravaginal misoprostol compared with the dinoprostone vaginal insert: a systematic review and metaanalysis. Am J Obstet Gynecol 2010; 202: 624.e1-624.e9
- 10 Souza AS, Amorim MM, Feitosa FE. Comparison of sublingual versus vaginal misoprostol for the induction of labour: a systematic review. BJOG 2008; 115: 1340-1349
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