To compare the effectiveness and convenience of a pen device for the self-administration of follitropin β with a conventional syringe delivering follitropin β solution in patients undergoing IVF-ET.
GnRH agonist long protocol was used for controlled ovarian stimulation (COS) in all subjects. A total of 100 patients were randomized into the pen device group or the conventional syringe group on the first day of COS. Local tolerance reactions were assessed within 5 minutes, at 1 hour and at 3 hours after each injection. On the day of hCG injection, patients were asked to rate their overall pain and convenience experienced with self-injection on a visual anlaogue scale (VAS).
There were no differences in patients' characteristics between the two groups. The duration of COS was significantly shorter in the pen device group than in the conventional syringe group. Patients included in the pen device group needed a significantly smaller amount of follitropin β. However, no differences between the two groups were found in IVF results and pregnancy outcome. The incidence of local pain within 5 minutes, at 1 hour and at 3 hours after the injection was significantly lower in the pen device group. VAS scores indicated that injections using the pen device were significantly less painful and more convenient.
The pen device for self-administration of follitropin β is less painful, safer and more convenient for the patients, and can be more effective because of the shorter duration and smaller dose of follitropin β when compared with the conventional syringe.
Urinary FSH had been replaced by recombinant human FSH (rhFSH) because rhFSH has a lower risk of immunogenicity and infection than that of the urinary products. Recombinant products are highly pure (>99%), and indeed, no antibodies to FSH have been detected in serum samples from patients who have injected rhFSH. Therefore, the use of this recombinant product has resulted in more efficient and predictable ovulation induction or controlled ovarian stimulation (COS). Additionally, rhFSH has been shown to be suitable for subcutaneous (SC) administration and SC injections allow for easy self-administration by patients [
RhFSH was first available as a freeze-dried lyophilized powder, which had to be dissolved in water for injection before administration. Recently, rhFSH has been made available as a premixed ready-to-use solution and this product has been considered more "patient friendly". A subsequent advance in patient-friendly regimens is the development of rhFSH solution, which is stored in cartridge form for administration with a pen device. This multiple-use pen device for SC self-administration of rhFSH, which is approved under the brand name Puregon Pen has been available in Europe since 2002. This pen injector is an adapted insulin pen, which has been shown to be better accepted by diabetes patients in comparison with conventional syringes, as it provides for an easier, safer, more accurate and more discrete insulin injection [
This study was performed to compare the effectiveness and convenience of a pen device for the self-administration of rhFSH (follitropin β) with a conventional syringe delivering rhFSH solution in patients undergoing COS for IVF-ET.
This study was a prospective, randomized, single center, group comparative study. A total of 100 infertile Korean women who were scheduled for IVF-ET with or without ICSI were enrolled in this study and they were divided into the pen device group or the conventional syringe group by a computer-generated randomization list using random numbers on the first day of COS. The patients were 20-39 years of age at the time of screening, and had normal ovulatory cycles (24-35 days in length), had a body mass index (BMI) between 18 and 29 kg/m2, and were willing to self-inject rhFSH.
Patients who had a history of current endocrine abnormalities, such as polycystic ovary syndrome, hyperprolactinemia, and a previous history of IVF-ET in which less than three oocytes were retrieved were excluded in this study. Patients who had any abnormalities that would interfere with adequate stimulation, previous hospitalization due to severe ovarian hyperstimulation syndrome (OHSS), history of previous (within 12 months) or current abuse of alcohol or drugs were also excluded from this study.
All patients received the same COS regimen, GnRH agonist luteal long protocol using triptorelin acetate (Decapeptyl; Ferring, Malmo, Sweden). After an absence of ovarian activity was confirmed by transvaginal ultrasound and/or serum estradiol levels after the administration of triptorelin acetate for at least 2 weeks, ovarian stimulation with rhFSH was carried out in both groups, starting with 200 or 250 IU follitropin β.
On the first day of ovarian stimulation, all subjects were randomized to self-administer rhFSH using a pen device (Puregon Pen; Organon, Oss, Netherland) equipped with a needle sized 29 G×13 mm or a conventional syringe equipped with a needle sized 25 G×16 mm by a computer generated randomization list using random numbers. On the first day of ovarian stimulation, patients were instructed how to self-inject subcutaneously into the abdominal wall around the umbilicus with a pen device or a conventional syringe and supervised in order to ensure correct self-injection.
After stimulation day 5, the dose of follitropin β was adjusted according to the individual ovarian response monitored by transvaginal ultrasound examinations. When one leading follicle reached 18 mm in diameter or 2 or more follicles reached 17 mm, oocyte maturation was triggered with 10,000 IU of hCG (Pregnyl; Organon) administered as a single intramuscular injection. Transvaginal ultrasound-guided oocyte retrieval was performed 36 hours after hCG administration. Embryos were transferred 3 days after oocyte retrieval. Luteal support was provided by administering 90 mg of vaginal progesterone gel (Crinone gel 8%; Serono SA, Geneva, Switzerland) once daily from the day of oocyte retrieval. Serum β-hCG levels were measured 11 or 12 days after embryo transfer. Pregnancies were confirmed by rising serum β-hCG concentrations and transvaginal ultrasonographic evidence of a gestational sac. If pregnancy was diagnosed, vaginal progesterone administration was continued for another 5 to 7 weeks. Clinical pregnancy was defined as the presence of a gestational sac by ultrasonography, while the miscarriage rate per clinical pregnancy was defined as the proportion of patients who failed to continue development before reaching 20 weeks of gestation among all clinical pregnancies.
After every injection of follitropin β, the severity of local tolerance symptoms was assessed by the patients themselves and recorded in a 'local tolerance diary book', within 5 minutes, at 1 hour and at 3 hours after injection. Local tolerance items scored were pain, redness, itching, bruising and swelling. The severity of symptoms was scored as none, mild, moderate, or severe. The incidence of each local tolerance item was compared between the pen device group and the conventional syringe group. Incidence indicates the percentage of subjects with mild, moderate or severe local tolerance symptoms for each item at each assessment. Additionally, on the day of hCG administration, patients were asked to rate their overall pain and convenience experienced with this self-injection method on a visual anlaogue scale (VAS). The VAS ranged from 0 (severe pain, not convenient) to 10 (no pain, very convenient).
The mean value was expressed as the mean±standard deviation (SD). A Student's
There were no differences in the age of patients and spouses, BMI, infertility duration, the rate of the patients with primary infertility, basal endocrine profile and indications for IVF/ICSI between the two groups (
The incidence of local pain within 5 minutes after injection was significantly lower in the pen device group (
The introduction of a pen device for the administration of recombinant insulin in the treatment of diabetes resulted in significant improvements for patients in terms of local discomfort, accurate dosing and convenience to the patients [
A previous study showed that injection pain is experienced less frequently when follitropin β is administered by a pen device than when follitropin α is administered with a conventional syringe [
None of the patients withdrew from our study because of the pain or other side effects. In addition, the incidence of severe OHSS was comparable between the two groups. Therefore, the pen device delivering rhFSH is judged to be at least as safe as the conventional syringe. Moreover, the present study demonstrated that the pen device is more convenient and easy to handle, when compared with the conventional syringe. The pen device delivering follitropin β permits accurate titration of rhFSH doses in increments of 25 IU. Individualized treatment for COS was therefore possible at the minimal effective dose.
In conclusion, the pen device for self-administration of follitropin β is safe, less painful and more convenient for patients undergoing COS, and can be more effective because of the shorter duration and smaller dose of follitropin β, when compared with a conventional syringe. A reduction of painful injections and the treatment period, and the convenient administration of rhFSH can make IVF treatment easier and more patient-friendly.
Presented at 61th Annual Meeting of American Society of Reproductive Medicine in Montreal, Canada.
This work was supported by the Organon grant 2003-0219.
No potential conflict of interest relevant to this article was reported.
Local tolerance reaction.
Patients' characteristics
Values are presented as mean±SD or number (%).
NS, not significant; BMI, body mass index; FSH, follicle stimulating hormone; LH, luteinizing; T, testosterone; SHBG, sex hormone binding globulin.
Comparison of controlled ovarian stimulation results and IVF outcome
Values are presented as number (%) or mean±SD.
ICSI, intracytoplasmic sperm injection; NS, not significant; COS, controlled ovarian stimulation; rhFSH, recombinant human follicle stimulating hormone; MII, metaphase II; OHSS, ovarian hyperstimulation syndrome.