Long-acting gonadotropin-releasing hormone agonists (GnRHa) are commonly used to treat central precocious puberty (CPP) in Korea. Although rare, there have been reports on the characteristic of adverse reactions of GnRHa in CPP among the Korean population. This study was intended to report on our clinical experience regarding significant adverse reactions to long-acting GnRHa in CPP and early onset puberty and to evaluate the prevalence rate of serious side effects.
This retrospective study included children with CPP and early onset puberty, who were administered monthly with long-acting GnRHa (leuprolide acetate, triptorelin acetate) at the outpatient clinic of Department of Pediatrics, at Inha University Hospital, between January 2011 and December 2013. We analyzed the clinical characteristics of patients who experienced significant adverse reactions and evaluated the prevalence rate.
Six serious side effects (0.9%) were observed among total of 621 CPP and early onset puberty children with GnRHa therapy. The number of sterile abscess formation was four in three patients (4 events of 621). Anaphylaxis occurred in only one patient, and unilateral slipped capital femoral epiphysis (SCFE) in another one patient. Anaphylaxis occurred after the 6th administration of the monthly depot triptorelin acetate. Unilateral SCFE developed in GnRHa therapy.
Sterile abscess formation occurred in 0.6% of CPP and early onset puberty patients from the administration of a monthly depot GnRHa therapy. The occurrences of anaphylaxis and SCFE are extremely rare, but can have serious implications on patients. Clinicians should be aware of these potential adverse effects related to GnRHa therapy in CPP.
Precocious puberty is defined as the occurrence of sexual maturation before the age of 8 years in girls and 9 years in boys. Central precocious puberty (CPP) is the gonadotropin-dependent form induced by the premature activation of the hypothalamic-pituitary-gonadal axis, due to various causes. The global secular decline in age at puberty has been recently reported with an increase in the number of children with CPP worldwide
Long-acting gonadotropin-releasing hormone agonists (GnRHa) are considered as a treatment for choice for pediatric CPP. Prolonged administration of GnRHa suppresses the pituitary-gonadal axis activity with a subsequent decrease of sex hormones. In Korea, monthly formulation of GnRHa, such as leuprolide acetate depot and triptorelin acetate depot, are widely used in children with CPP. The number of children treated with CPP using these drugs has gradually increased due to an increase in the number of girls referred for evaluation of CPP
Although local side effects, including pain, flares and subcutaneous nodules have been known, long-acting formulations of GnRHa are well tolerated in children. However, sterile abscess formation related to GnRHa can be one of the most significant adverse drug reactions that greatly affect the compliance with the treatment. Sterile abscess formation has been generally reported as 1.5%-3% of all patients with monthly depot GnRHa therapy
The purpose of this study was intended to report our clinical experience with significant adverse reactions to long-acting GnRHa in CPP at single pediatric tertiary medical center and to evaluate the prevalence rate of serious side effects.
This study was conducted to report on those patients who experienced severe adverse effects among the total CPP and early onset puberty patients who were administered monthly long-acting GnRHa (leuprolide acetate, triptorelin acetate) at the outpatient clinic at Department of Pediatrics, Inha University Hospital, from January 2011 to December 2013. We analyzed the clinical characteristics of patients who experienced significant adverse reactions and evaluated the prevalence rate.
The subjects' medical records were reviewed retrospectively. Information regarding gender, age, height, weight, pubertal stage, bone age, serum hormone levels including luteinizing hormone (LH), follicle-stimulating hormone (FSH), and estradiol (E2) were recorded. In addition, drug type of GnRHa used for therapy, injection dose and interval, onset of occurrence of adverse reaction, clinical course of adverse reaction, and past allergy history were recorded.
The definitions of terms are as follows. CPP is the onset of signs of puberty before the age of 8 years in girls and 9 years in boys, the result of early maturation of the hypothalamic-pituitary-gonadal axis. Early onset puberty is defined as the occurrence of sexual maturation after the age of 8 years and before 9 years in girls, after 9 years and before 10 years in boys. Sterile abscess is defined as an abscess with contents that are not caused by pyogenic bacteria. Anaphylaxis is a serious allergic or hypersensitivity reaction that is rapid in onset and may cause life-threatening conditions
Among the total 621 patients, 469 girls (8.78±0.45 years) were treated with monthly depot leuprolide acetate, of which, 152 girls (8.35±0.47 years) were treated with monthly depot triptorelin acetate. Drug-related serious side effects were observed in 6 events within 5 girls among the total patients (0.9%). In 4 events out of 621 patients, sterile abscess resulted from an administration of GnRHa, which demonstrated 0.6% prevalence rate. Anaphylaxis happened in one patient, and unilateral SCFE in another patient relatively (
This 7.6-year-old girl was an otherwise healthy diagnosed with CPP following presentation of an 8-month history of breast development (Tanner stage 3) with growth spurt. Her height was 130.3 cm (50th-75th percentile), and weight was 30 kg (50th-75th percentile). Her bone age was 10 years by the Greulich and Pyle method at a chronological age of 7.85 years. GnRH stimulation test demonstrated a dominant LH response; peak LH level, 7.5mIU/mL; peak FSH level, 8.2 mIU/mL. Luprolide acetate depot (Leuplin, Takeda pharmaceuticals Korea, Seoul, Korea) therapy began with subcutaneously (SC) injection every 4 weeks. After the second injection, she had heat sensation at the injection site and a mass was formed. Following the seventh injection, erythematous plaques with sterile abscess (size: 15 mm×20 mm, 5 mm×5 mm) were developed at the injection site after three weeks. The drug has been switched to triptorelin acetate depot (Decapeptyl, Ferring pharmaceuticals, Seoul, Korea) intramuscularly (IM) injection without further problems. The abscess local lesion was healed after spontaneous rupture of abscess (
An 8.9-year-old girl was presented with 10 months of breast development (Tanner stage 3). Height was 134.3 cm (25th-50th percentile) and weight was 29.5 kg (25th-50th percentile), but an increase in growth velocity over 6 months showed. Random serum levels of LH, FSH, E2 were 2.4 mIU/mL (normal, <0.3 mIU/mL), 5.03 mIU/mL (normal, 1.0-4.2 mIU/mL), and 45.18 pg/mL (normal, <10 pg/mL), respectively. Her bone age was advanced at 10 years. Leuprolide acetate depot (Luphere, Daewoong pharmaceutical, Seoul, Korea) initiated SC monthly injection. Following the ninth injection of leuprolide acetate depot SC, she developed a painful erythematous change at the injection site, consistent with sterile abscess. The lesion gradually healed without any scarring. After the therapy was changed to triptorelin acetate depot (Decapeptyl) IM injection, there has been no particular local site events.
An otherwise healthy 9-year-old girl visited the hospital due to an 8-month history of progressive breast development (Tanner stage 3) with pubic hair (Tanner stage 2): random LH, 1.8 mIU/mL; FSH, 1.6 mIU/mL; E2, 12.7 pg/mL. Her height was 140.5 cm (75th-90th percentile), and weight was 41 kg (90th-95th percentile). Her bone age was 11 years. Luprolide acetate depot (Luphere) administered with a diagnosis with early onset puberty. After the fifth injection, a sterile abscess formation (size, 20 mm×15 mm) with pus occurred at the injection site. Recurrent abscess developed and it was frequently drained from the injection site. Eight weeks later, the wound healed with little scarring. Thereafter, the treatment of drug was changed to triptorelin acetate depot (Decapeptyl), which was IM injected in the buttock. The injection therapy was stopped due to a sterile abscess with pus (size, 20 mm×15 mm) that occurred again at the injection site after the first triptorelin acetate depot shot. The lesion on her buttock healed leaving a residual scarring (size, 10 mm×10 mm) 10 weeks later (
An 8.4-year-old girl was presented with breast development (Tanner stages 2, 3) and pubic hair (Tanner stage 2) over the preceding 10 months. She had neither a specific medical history nor history of allergic disorder. Her height was 135.7 cm (90th-95th percentile), and weight was 31.4 kg (70th-90th percentile). Her bone age was 10 years. GnRH stimulation testing showed the diagnosis of early puberty with LH peaking at 32.6 mIU/mL and FSH peaking at 28.5 mIU/mL. She was treated with triptorelin acetate depot (Decapeptyl) SC injected at four-week intervals. Immediately after the sixth injection, she developed dizziness, headache, whole body redness, and chest tightness. Subsequently, she lost consciousness. Blood pressure (BP) could not be measured at that time. All of the above symptoms were relieved within several minutes without any particular treatment. Her BP measured after the recovery was 99/56 mmHg which was a low-normal level (systolic, 25th-50th percentile; diastolic, 25th-50th percentile). Her ordinary BP was 110/60 mmHg (systolic, 50th-75th percentile; diastolic, 75th-90th percentile). Anaphylaxis was considered to have occurred, and the drug therapy was changed into a monthly SC injection of leuprolide acetate depot (Leuplin). She maintained this monthly leuprolide therapy without further systemic adverse reactions.
A 9-year-old girl visited the hospital due to a 6-month history of progressive breast development (Tanner stage 3). She had no specific medical history. Her height was 140 cm (75th-90th percentile), weight was 38 kg (75th-90th percentile), and body mass index
Neely et al.
In this study, sterile abscesses formations occurred in 0.6% of CPP and early onset puberty patients with GnRHa therapy. Out of a total of 469 patients with leuprolide acetate depot, three events (0.6%), while in one event (0.6%) out of a total of 152 patients with triptorelin acetate depot. In the first and second cases, sterile abscess formation occurred under leuprolide acetate therapy, and abscess did not occur after being changed into triptorelin acetate. In case 3, sterile abscesses not only occurred following leuprolide acetate depot therapy, but also developed even after a switch to another GnRHa, triptorelin acetate depot.
The postulated cause for these reactions is likely to be antibody formation against the biodegradable polymers, which deliver GnRHa drug in a long-acting manner
While sterile abscesses are rare, such reaction can induce great anxiety to patients and families. These reactions may often persist for several months and can leave significant scarring such as our third case. These formations can also cause the failure of GnRHa therapy. Also, these effects may determine treatment interruption. Clinicians should be aware of the chance of adverse reactions following the treatment of GnRHa depot.
There are several reports of anaphylaxis to GnRHa in Western countries. Grant and Levinson
According to the guidelines for anaphylaxis published in 2006, anaphylaxis can be diagnosed if there are two or more symptoms, such as involvements of the skin-mucosal tissue, respiratory compromise, reduced BP or associated symptom, and persistent gastrointestinal symptoms after exposure to any allergen
SCFE is an early adolescent hip disorder; the femoral head is separated from the femoral metaphysis. This disorder mainly occurs in those aged 10-15 years more frequently in males and its incidence rate is assumed to be one out of 10,000 persons
There have been a few published reports regarding SCFE occurrence on or after cessation of GnRHa treatment
Our fifth case was not obese and had no other hormonal disorder except early onset puberty. Most children with SCFE in other studies were different from ours in that GnRHa therapy was involved for a longer time because of earlier onset age of CPP. In case5, SCFE seems to occur coincidentally following GnRHa therapy. However, GnRHa treatment for CPP may be considered as a risk factor affecting the development of SCFE. Further studies seem to be necessary on the relationship between the occurrence of SCFE and GnRHa therapy.
In conclusion, in this study, sterile abscess formation occurred in 0.6% of CPP and early onset puberty patients with monthly depot GnRHa therapy. We also experienced the rare occurrence of one case of anaphylaxis, and another case of SCFE following GnRHa treatment in CPP and early onset puberty. GnRHa have been widely used globally and their drug safety has been well established. However, as the number of patients with GnRHa therapy is on the rise, potential adverse drug reactions can be increasing in number. Clinicians should be well acquainted with the potential adverse effects related to GnRHa therapy in CPP. Further studies are necessary to identify the mechanisms of development of potential adverse drug reactions.
No potential conflict of interest relevant to this article was reported.
Leuprolide acetate depot was subcutaneously injected into the upper arm of a 7.6-year- old girl at four-week interval. A sterile abscess was formed at the injection site after the 7th injection.
Leuprolide acetate depot was subcutaneously injected into the arm of a 9-year-old girl at four-week interval. (A) A sterile abscess was formed at the injection site after the 5th injection. (B) The treatment was switched to triptorelin depot, which intramuscularly injected into her buttock, but a sterile abscess and pus formed 3 weeks after the first injection. (C) The lesion on the buttock healed with scarring 10 weeks later.
Characteristics of patients with central precocious puberty and early onset puberty showing serious adverse drug reactions
Patient No. | Age (yr) | Bone age (yr) | Sex | Adverse drug reaction | GnRHa depot | Interval (wk) | Onset of event | Allergic history |
---|---|---|---|---|---|---|---|---|
1 | 7.6 | 10.0 | F | Sterile abscess | Leuprolide | 4 | 7th Injection | None |
2 | 8.9 | 10.0 | F | Sterile abscess | Leuprolide | 4 | 9th Injection | None |
3 | 9.0 | 11.0 | F | Sterile abscess (1st) | Leuprolide | 4 | 5th Injection | None |
Sterile abscess (2nd) | Triptorelin | 4 | 1st Injection | |||||
4 | 8.4 | 10.0 | F | Anaphylaxis | Triptorelin | 4 | 6th Injection | None |
5 | 9.0 | 11.5 | F | SCFE | Leuprolide | 4 | 5th Injection | None |
Triptorelin | 4 | 6th Injection |
GnRHa, gonadotropin-releasing hormone agonist; SCFE, slipped capital femoral epiphysis.
Reports of luteinizing hormone releasing hormone analogs and "immune systems disorders" 1988-2010 of World Health Organization (97 countries) [
Drug | Reaction | No. of reports |
---|---|---|
Leuprolide | Anaphylactic shock |
7 |
Anaphylactic reaction |
4 | |
Anaphylactoid reaction |
23 | |
Serum sickness |
6 | |
Multiple allergies | 1 | |
Hypersensitivity |
66 | |
Allergy to metals | 1 | |
Triptorelin | Anaphylactic shock |
3 |
Anaphylactic reaction |
2 | |
Anaphylactoid reaction |
1 | |
Hypersensitivity |
5 |
Definitions conform the Netherlands Pharmacovigilance Center Lareb.
Hypersensitivity reaction with clinical signs in 2 or more organ systems with low blood pressure.
Hypersensitivity reaction with clinical signs in 2 or more organ system without low blood pressure.
Nonallergic anaphylactic shock or reaction.
Serum sickness is a reaction similar to an allergy. Specifically, it is an immune system reaction to certain medications, injected proteins or antiserum.
Symptoms being an expression of hypersensitivity.