Introduction
Precocious puberty is defined as the development of secondary sexual characteristics earlier than two standard deviations of the mean value
1). It occurs at least 10 times more frequently in girls than in boys. The clinical manifestations in girls with precocious puberty are breast development before 8 years. Public interest in precocious puberty is gradually increasing because it can cause psychological discrepancies between physical and chronologic age, and it may increase the risks for social problems such as school violence and sexual abuse
2). Moreover, precocious puberty can cause a shorter final height due to the early closure of the epiphyses.
Precocious puberty may be classified into two groups, which are central precocious puberty (CPP, also known as true precocious puberty) and peripheral precocious puberty (also known as precocious pseudopuberty). CPP is the result of the precocious activation of the hypothalamic-pituitary-gonadal axis, and the majority of CPP is idiopathic, which is commonly treated with gonadotropin-releasing hormone agonists (GnRHa)
3).
GnRHa is generally considered standard treatment for CPP. It reduces gonadotropin release selectively and lowers sex steroid hormone secretion to a prepubertal level
4). In detail, GnRHa acts via desensitization and down-regulation of pituitary GnRH receptors and as a result gonadotropin release is gradually inhibited after an initial stimulation 'flare-up' phase
5). GnRHa treatment is reported to be effective in postponing pubertal development by slowing the accelerated growth and bone maturation, thus preserving height potential
3). However, there is still controversy over the benefits and effects of GnRHa treatment, especially about the preservation of adult height (AH)
6).
The aim of the present study was to evaluate the statural growth outcomes in girls with CPP who were treated with GnRHa with or without growth hormone (GH). We analyzed height preservation by assessing the changes in height standard deviation score (SDS) for bone age (BA), and comparing their AHs with their midparental height (MPH) and predicted adult height (PAH) prior to GnRHa treatment initiation.
Materials and methods
1. Subjects
We retrospectively analyzed the medical records of the 82 girls with idiopathic CPP who were treated with GnRHa and attained their final AHs at the Pediatric Endocrinology Clinic of Severance Hospital from 2004 to 2014. As some of these patients had also received GH treatment, we divided the patients into two groups, one group received GnRHa treatment alone (n=59) and the other group receiving GnRHa plus GH treatment (n=23).
Patients were identified to have idiopathic CPP if they satisfied the classical diagnostic criteria: (1) the onset of breast development (Tanner stage B2 or above) before the age of eight, (2) peak luteinizing hormone (LH) level of above 5 IU/L in the standard intravenous GnRH stimulation test, and (3) no evidence of hypothalamic-pituitary organic lesions, confirmed by magnetic resonance imaging. Subjects were excluded from analysis if they had any additional conditions that could affect the onset of puberty such as hypothyroidism or congenital adrenal hyperplasia.
2. Methods
Subcutaneous injections of GnRHa were administered to the patients at a dose of 75-150 µg/kg every 28 days. Twenty-eight percent of patients (23 of 82 CPP girls) underwent GnRHa and GH combined treatment. In the GH combined group, patients were treated with subcutaneous injection of GH at a dose of 0.25 mg/kg per week, 6 days weekly. The GH treatment duration was 1.9±0.99 years (0.6-4.1 years).
We evaluated height, weight, body mass index (BMI) and BA before and after GnRHa treatment. At each evaluation, height was measured three times with a Harpenden stadiometer. The BA was assessed by the Greulich-Pyle method
7) by the same observer. Growth parameters such as height, weight, and BMI were expressed as SDS, which was calculated using the Korean children and adolescents growth standard
8). PAH was calculated according to the Bayley-Pinneau method
9). MPH was defined as the average of the parental heights minus 6.5 cm. AH was measured at the time when growth velocity was less than 1 cm per year, at least two years after menarche, and when BA was over 15 years. Also, gain of height SDS (difference between AH SDS and initial height SDS for BA), AH-MPH (difference values between AH and MPH), and AH-PAH at start (difference between AH and initial PAH) were analyzed to assess the effectiveness of GnRHa.
The serum levels of LH, FSH were measured by sequential two-step immunoenzymatic assay (Access hLH, FSH Reagent Pack, Beckman Coulter Inc., Brea, CA, USA), and E2 level was measured using a competitive binding immunoenzymatic assay (Access Estradiol Reagent, Beckman Coulter Inc.).
3. Statistical analysis
Statistical analysis of the results was performed using IBM SPSS Statistics ver. 20.0 (IBM Co., Armonk, NY, USA). All data was expressed as mean±standard deviation, and the paired t-test was applied to compare the data. Correlations between parameters were determined using Pearson correlation coefficient analysis. A P-value of less than 0.05 was considered statistically significant.
Results
1. Auxological characteristics of subjects treated with GnRHa alone during treatment and at AH
Chronological age (CA) and BA at the start of GnRHa treatment were 8.7±0.78 and 10.2±1.60 years, respectively. BA was advanced 1.7±0.58 years compared to CA. At the end of treatment, BA was 11.9±0.54 years, the difference between BA and CA was 1.3±0.63 years, which was lower than the difference at the start of treatment (
P<0.001) (
Table 1). This result suggested that GnRHa treatment had an effect on postponing bone maturation. Height SDS adjusted for BA was increased during treatment and at AH; it was -0.4±0.81 at the start, -0.3±0.80 at the end of treatment, and 0.3±0.87 at final (
Table 1,
Fig. 1). The difference values from the start of treatment were 0.1±0.42 at the end of treatment (
P=0.056), and 0.7±0.82 at AH (
P<0.001). This result showed that compared to the initial measurements, height SDS for BA increased significantly at final AH, whereas it was not significantly different during GnRHa treatment. AH (160.4±4.23 cm) was significantly higher than the initial PAH (156.6±3.96 cm) (AH-PAH was 3.8±4.03 cm,
P<0.001), and similar to MPH (159.9±3.52 cm) (
Table 1.
Fig. 2).
2. Auxological characteristics of subjects treated with
GnRHa plus GH during treatment and at AH
BA at the start of treatment was 10.5±0.86 years, which was 1.7±0.69 years more than CA, whereas BA at the end of treatment was 11.9±0.43 years, which was 1.2±0.62 years more than CA. The difference between BA and CA at the end of treatment was also lower than before treatment, similar to the GnRHa alone group (
P<0.001) (
Table 2). Height SDS for BA was also increased during treatment and at AH. It indicated -1.0±0.53 before treatment, -0.5±0.82 at the end of treatment, and 0.1±1.10 at AH (
Table 2,
Fig. 1). The difference values from the start were 0.5±0.64 at the end of treatment (
P<0.001), and 1.1±1.05 at AH (
P <0.001). This result showed that the height SDS for BA in the GH combined group constantly increased during treatment. AH (159.3±5.33 cm) reached MPH (158.1±3.31 cm), and was significantly higher than the initial PAH (154.6±2.55 cm) (AH-PAH was 4.7±5.04 cm,
P<0.001) (
Table 2,
Fig. 2).
3. Comparison of growth outcomes between GnRHa alone group and GnRHa plus GH group
Gain of height SDS (difference between AH SDS and initial height SDS for BA) were 1.0±0.91 in GnRHa alone group and 1.2±0.93 in GnRHa plus GH group, showing no significant difference between the two groups (
P=0.44) (
Table 3). It could be explained that the height gain was slightly higher in the GH combined group, but it was not to be a statistically significant level. In addition, AM-MPH (0.5±4.11 cm in GnRHa alone vs. 1.2±5.47 cm in the GH combined group,
P=0.53) and AH-PAH at start (3.8±4.03 cm in GnRHa alone vs. 4.7±5.06 cm in the GH combined group,
P=0.43) presented no significant difference between two groups (
Table 3).
4. The correlation between AH and other auxological factors
Multiple regression analysis was done to find the factors to influence the growth outcomes on AH SDS (
Table 4). The GH combined group was excluded, since GH could be a compounding factor. The AH SDS showed statistically positive effects when the CA at start was younger, MPH was taller. The BA at start, BA-CA at start, PAH at start, height SDS at start, and duration of treatment had no correlation with the growth outcome.
5. Time of menarche and growth pattern after cessation of GnRHa
The time of menarche and the growth pattern after cessation of GnRHa treatment were analyzed (
Table 5). Duration from cessation of GnRHa to menarche was 1.0±0.61 years. Height increment from cessation of GnRHa to menarche was 5.9±3.65 cm, whereas the height increment after menarche was 7.1±2.25 cm. Thus, height increment from cessation of GnRHa to final AH was 13.0±4.31 cm.
Discussion
The timing of normal puberty has shown a dramatic decline in age during past centuries. Moreover, the number of patients with CPP has been significantly increased recently. This trend also occurred in Korea with a four- to five-fold increase of CPP in girls over the last five years
10). CPP may cause physical and psychological problems for affected girls, so some girls with CPP could be at risk of premature sexual activity, and consequently, sexual abuse. Some reports have shown increased behavioral disturbances, including drug abuse and low socio-culture outcomes
11). Therefore, proper treatment for CPP is important, not only for individuals but also for society.
GnRHa is generally accepted as the treatment of choice for the improvement of final AH preservation and also for the reduction of psychosocial problems in CPP patients, however controversy still exists over whether GnRHa treatment improves final AH. Lazar et al.
12) found that GnRHa treatment results in little or no increase in final AH when treatment is initiated after eight years of age. In a study by Pasquino et al.
13) in which 87 GnRHa-treated (age, 6.5 years) and 32 nontreated girls with idiopathic CPP (age, 6.8 years), the final AH of treated and nontreated girls were 159.8 and 154.4 cm, respectively. Heger et al.
14) also reported on 50 girls with precocious puberty undergoing GnRHa treatment for two years, whose final AH averaged 160.6±8.0 cm (-0.6±1.3 SDS), which was significantly higher than the initial PAH of 154.9±9.6 cm. Our 82 GnRHa-treated CPP girls achieved final heights that were significantly greater than their pretreatment PAH, which is in agreement with recent studies. In our study, height gain was approximately 3.8 cm in the GnRHa alone group, while 4.7 cm in the GH plus group. In addition, AH showed a taller tendency when the CA at start was younger and MPH was taller.
Another issue of this study is whether combined GH treatment improves the growth outcomes of CPP girls. There have been few previous studies about the effectiveness of GH combined therapy on growth outcomes. Pasquino et al.
15) and Pucarelli et al.
16) showed differences of about 6-8 cm of height gain on girls with CPP treated with GnRHa plus GH were noted, compared to GnRHa alone. Until the present, there have been no definite conclusions about the growth outcomes of GH-combined treatments. In this study, gain of height SDS and difference between AH and initial PAH were slightly higher in the GnRHa plus GH group than in the GnRHa alone group in CPP girls, however it showed no statistically significant difference between two groups. These results suggested that combined GH treatment showed a limited increase in height gain. Growth pattern between two groups showed that height SDS for BA was continuously increased during treatment and at AH in the GnRHa plus GH group, whereas it was increased only at AH in the GnRHa alone group. This result may result from several reasons. One possibility is that the choice of GH treatment might have a selection bias. Those who have low height potential or attenuated growth velocity might tend to choose the combined GH treatment. Because GH treatment requires the consideration of cost, economic status may be another affecting factor to select the patients treated with GnRHa plus GH. Furthermore, GH treatment duration could be another influencing factor. Cost-effectiveness of combined GH treatment in patients with CPP has to be elucidated.
The suppression of the hypothalamic-pituitary-gonadal axis was fully recovered after discontinuation of GnRHa. The average time span from the cessation of treatment to menarche was 1.0 years. Our data about the growth pattern after cessation of GnRHa can be helpful to predict the height increase after discontinuation of GnRHa. In addition, there have been conflicting data regarding the increase in obesity during GnRHa treatment
17). In present study, the BMI score of girls treated with GnRHa was not significantly increased during treatment. In addition, no adverse effects have been observed.
There were some limitations in our study. GnRHa treatment is not an only single factor to determine the growth outcomes, rather the effects of nutrition, psychosocial status, genetic height potential, and others may influence the outcome. Because GnRHa has recently been accepted as the standard therapy for CPP, GnRHa-untreated patients could not be enrolled in this study. Furthermore, it is considered that further studies about the growth outcomes in CPP girls treated with GnRHa plus GH are required.
In this study about GnRHa treatment in CPP girls, the final AH was significantly higher than the initial height predictions and was close to the MPH. Therefore, it can be concluded that GnRHa treatment is helpful to improve the growth outcomes in girls with CPP.