Kombinirana oralna hormonska kontracepcijska pilula za primarnu dismenoreju
Abstract
Background
Dysmenorrhoea (painful menstrual cramps) is common and a major cause of pain in women. Combined oral contraceptives (OCPs) are often used in the management of primary dysmenorrhoea, but there is a need for reporting the benefits and harms. Primary dysmenorrhoea is defined as painful menstrual cramps without pelvic pathology.
Objectives
To evaluate the benefits and harms of combined oral contraceptive pills for the management of primary dysmenorrhoea.
Search methods
We used standard, extensive Cochrane search methods. The latest search date 28 March 2023.
Selection criteria
We included randomised controlled trials (RCTs) comparing all combined OCPs with other combined OCPs, placebo, or management with non‐steroidal anti‐inflammatory drugs (NSAIDs). Participants had to have primary dysmenorrhoea, diagnosed by ruling out pelvic pathology through pelvic examination or ultrasound.
Data collection and analysis
We used standard methodological procedures recommended by Cochrane. The primary outcomes were pain score after treatment, improvement in pain, and adverse events.
Main results
We included 21 RCTs (3723 women). Eleven RCTs compared combined OCP with placebo, eight compared different dosages of combined OCP, one compared two OCP regimens with placebo, and one compared OCP with NSAIDs.
OCP versus placebo or no treatment
OCPs reduce pain in women with dysmenorrhoea more effectively than placebo. Six studies reported treatment effects on different scales; the result can be interpreted as a moderate reduction in pain (standardised mean difference (SMD) −0.58, 95% confidence interval (CI) −0.74 to −0.41; I² = 28%; 6 RCTs, 588 women; high‐quality evidence). Six studies also reported pain improvement as a dichotomous outcome (risk ratio (RR) 1.65, 95% CI 1.29 to 2.10; I² = 69%; 6 RCTs, 717 women; low‐quality evidence). The data suggest that in women with a 28% chance of improvement in pain with placebo or no treatment, the improvement in women using combined OCP will be between 37% and 60%.
Compared to placebo or no treatment, OCPs probably increase the risk of any adverse events (RR 1.31, 95% CI 1.20 to 1.43; I² = 79%; 7 RCTs, 1025 women; moderate‐quality evidence), and may also increase the risk of serious adverse events (RR 1.77, 95% CI 0.49 to 6.43; I² = 22%; 4 RCTs, 512 women; low‐quality evidence).
Women who received OCPs had an increased risk of irregular bleeding compared to women who received placebo or no treatment (RR 2.63, 95% CI 2.11 to 3.28; I² = 29%; 7 RCTs, 1025 women; high‐quality evidence). In women with a risk of irregular bleeding of 18% if using placebo or no treatment, the risk would be between 39% and 60% if using combined OCP. OCPs probably increase the risk of headaches (RR 1.51, 95% CI 1.11 to 2.04; I² = 44%; 5 RCTs, 656 women; moderate‐quality evidence), and nausea (RR 1.64, 95% CI 1.17 to 2.30; I² = 39%; 8 RCTs, 948 women; moderate‐quality evidence). We are uncertain of the effect of OCP on weight gain (RR 1.83, 95% CI 0.75 to 4.45; 1 RCT, 76 women; low‐quality evidence). OCPs may slightly reduce requirements for additional medication (RR 0.63, 95% CI 0.40 to 0.98; I² = 0%; 2 RCTs, 163 women; low‐quality evidence), and absence from work (RR 0.63, 95% CI 0.41 to 0.97; I² = 0%; 2 RCTs, 148 women; low‐quality evidence).
One OCP versus another OCP
Continuous use of OCPs (no pause or inactive tablets after the usual 21 days of hormone pills) may reduce pain in women with dysmenorrhoea more effectively than the standard regimen (SMD −0.73, 95% CI −1.13 to 0.34; 2 RCTs, 106 women; low‐quality evidence). There was insufficient evidence to determine if there was a difference in pain improvement between ethinylestradiol 20 μg and ethinylestradiol 30 μg OCPs (RR 1.06, 95% CI 0.65 to 1.74; 1 RCT, 326 women; moderate‐quality evidence). There is probably little or no difference between third‐ and fourth‐generation and first‐ and second‐generation OCPs (RR 0.99, 95% CI 0.93 to 1.05; 1 RCT, 178 women; moderate‐quality evidence). The standard regimen of OCPs may slightly increase the risk of any adverse events over the continuous regimen (RR 1.11, 95% CI 1.01 to 1.22; I² = 76%; 3 RCTs, 602 women; low‐quality evidence), and probably increases the risk of irregular bleeding (RR 1.38, 95% CI 1.14 to 1.69; 2 RCTs, 379 women; moderate‐quality evidence). Due to lack of studies, it is uncertain if there is a difference between continuous and standard regimen OCPs in serious adverse events (RR 0.34, 95% CI 0.01 to 8.24; 1 RCT, 212 women), headaches (RR 0.94, 95% CI 0.50 to 1.76; I² = 0%; 2 RCTs, 435 women), or nausea (RR 1.08, 95% CI 0.51 to 2.30; I² = 23%; 2 RCTs, 435 women) (all very low‐quality evidence).
We are uncertain if one type of OCP reduces absence from work more than the other (RR 1.12, 95% CI 0.64 to 1.99; 1 RCT, 445 women; very low‐quality evidence).
OCPs versus NSAIDs
There were insufficient data to determine whether OCPs were more effective than NSAIDs for pain (mean difference −0.30, 95% CI −5.43 to 4.83; 1 RCT, 91 women; low‐quality evidence). The study did not report on adverse events.
Authors' conclusions
OCPs are effective for treating dysmenorrhoea, but they cause irregular bleeding, and probably headache and nausea. Long‐term effects were not covered in this review. Continuous use of OCPs was probably more effective than the standard regimen but safety should be ensured with long‐term data. Due to lack of data, we are uncertain whether NSAIDs are better than OCPs for treating dysmenorrhoea.
PICOs
Laički sažetak
Kombinirana oralna hormonska kontracepcijska pilula (OHK) u liječenju primarne dismenoreje
Istraživačko pitanje
Cochraneovi autori pregledali su dokaze o učinkovitosti i sigurnosti kombiniranih oralnih hormonskih kontracepcijskih pilula (OHK‐a) za liječenje bolnih menstrualnih grčeva (menstrualnih bolova, koji se nazivaju i dismenoreja).
Dosadašnje spoznaje
Kombinirane oralne hormonske kontracepcijske pilule (OHK) već se koriste za liječenje menstrualnih grčeva, ali dokazi o njihovoj učinkovitosti nisu bili uvjerljivi.
Značajke istraživanja
Pronađeno je 21 randomizirano kontrolirano istraživanje (klinička ispitivanja u kojima se ljude nasumično svrstava u jednu ili više istraživačkih skupina) u kojima se uspoređivalo učinke OHK‐a ili s placebom (lažnom pilulom), drugim OHK‐om, ili nesteroidnim protuupalnim lijekovima koji smanjuju bol i upalu. U istraživanjima su sudjelovale 3723 žene. Većina žena imala je bolne menstrualne grčeve barem umjerene jačine. Proizvođači OHK‐a financirali su 11 ispitivanja. Baze podataka pretražene su u ožujku 2023. godine.
Ključni rezultati
OHK u usporedbi s placebom
OHK smanjuje bol za 0,7 do 1,3 boda na ukupnoj ljestvici dismenoreje (raspon od 0 do 6) više od placeba kod žena s menstrualnim grčevima (6 istraživanja s 588 sudionica; visoka kvaliteta dokaza). U šest istraživanja u kojima se poboljšanje simptoma mjerilo s da/ne pitanjima, pokazalo se da OHK može umanjiti bol. Žene koje imaju 28% šanse za poboljšanje simptoma uz placebo mogu imati 37% do 60% šanse za poboljšanje uz OHK (dokazi niske kvalitete).
OHK povećava rizik od nuspojava (59% u placebo skupini u usporedbi sa 71% do 86% u OHK skupini; dokazi srednje razine kvalitete) te može dovesti do ozbiljnijih nuspojava (1,1% u placebo skupini u usporedbi s 0,5% do 6,8% u OHK skupini; dokazi niske kvalitete).
Neredovito krvarenje povećava se kod žena koje uzimaju OHK. Žene kod kojih je rizik od neredovitog krvarenja 18% uz placebo imaju rizik od neredovitog krvarenja od 39% do 60% uz OHK (dokazi visoke kvalitete). Dokazi umjerene kvalitete pokazali su da OHK vjerojatno povećava rizik od glavobolja (17% u placebo skupini u usporedbi s 19% do 35% u OHK skupini) i mučnine (10% u placebo skupini u usporedbi s 11% do 22% u OHK skupini).
Učinak OHK‐a na dobitak kilograma nije siguran.
Dokazi niske kvalitete pokazali su da OHK može blago smanjiti potrebu za dodatnim lijekovima (38% u placebo skupini u usporedbi s 15% do 37% u OHK skupini) i odsutnost s posla (36% u placebo skupini u usporedbi s 11% do 35% u OHK skupini).
Usporedba različitih vrsta OHK‐a
Može postojati mala ili nikakva razlika između OHK‐a koji sadrži niske ili visoke doze estrogena, ili između novijih i starijih formula OHK‐a (dokazi umjerene kvalitete).
Korištenje kontinuirane oralne hormonske kontracepcije (bez neaktivnih tableta koje se uzimaju u pauzi između aktivnih tableta, kako bi se odgodilo mensturalno krvarenje) može umanjiti bol više od tradicionalnog režima (dokazi niske kvalitete). Tradicionalni režim je uzimanje aktivnih tableta 21 dan i pauza od 7 dana (ili uzimanje neaktivnih tableta 7 dana), gdje se obično javlja probojno menstrualno krvarenje.
Može postojati mala ili nikakva razlika u riziku od bilo koje nuspojave između kontinuiranog i tradicionalnog režima (65% u tradicionalnoj skupini u usporedbi sa 66% do 80% u kontinuiranoj skupini; dokazi niske kvalitete).
Zbog vrlo niske kvalitete dokaza, nije sigurno postoji li razlika u riziku od ozbiljnih nuspojava (0,9% u tradicionalnoj skupini u usporedbi s 0,3% do 7,7% u kontinuiranoj skupini), broju glavobolja (8% u tradicionalnoj skupini u usporedbi s 4% do 15% u kontinuiranoj skupini), mučnina (6% u tradicionalnoj skupini u usporedbi s 3% do 13% u kontinuiranoj skupini) ili odsutnosti s posla (9% u tradicionalnoj skupini u usporedbi s 6% do 18% u kontinuiranoj skupini). Kontinuirana uporaba OHK‐a vjerojatno pogoršava neredovito krvarenje (33% u tradicionalnoj skupini u usporedbi s 38% do 56% u kontinuiranoj skupini; dokazi srednje razine kvalitete).
U ovim istraživanjima nisu praćeni dobitak kilograma ni potreba za dodatnim lijekovima.
OHK u usporedbi s nesteroidnim protuupalnim lijekovima
Zbog niske kvalitete dokaza nije utvrđeno je li oralna hormonska kontracepcija učinkovitija od nesteroidnih protuupalnih lijekova. Nisu zabilježene nuspojave.
Kvaliteta dokaza
Kvaliteta dokaza kretala se od vrlo niske do visoke. Najvažniji problemi bili su nedostatak podataka i razlike u podacima između istraživanja.
