Yava� �lerleyen ve H�zl� �lerleyen Santral Puberte Prekoks Olan K�zlar�n Kar��la�t�rmal� Analizi: Tek Merkez Deneyimi

Tetik Dincer, B�sra; Dagdeviren Cak�r, Aydilek; Ucar, Ahmet

Cilt : 59 Say� : 3 Y�l : 2025

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Yava� �lerleyen ve H�zl� �lerleyen Santral Puberte Prekoks Olan K�zlar�n Kar��la�t�rmal� Analizi: Tek Merkez Deneyimi [Med Bull Sisli Etfal Hosp]

Med Bull Sisli Etfal Hosp. 2025; 59(3): 360-365 | DOI: 10.14744/SEMB.2024.56957

Yava� �lerleyen ve H�zl� �lerleyen Santral Puberte Prekoks Olan K�zlar�n Kar��la�t�rmal� Analizi: Tek Merkez Deneyimi

B�sra Tetik Dincer¹, Aydilek Dagdeviren Cak�r², Ahmet Ucar²
¹Pediatri Anabilim Dal�, Dr. Sami Ulus �ocuk Sa�l�� ve Hastal�klar� E�itim ve Ara�t�rma Hastanesi, Ankara, T�rkiye
²Pediatri Anabilim Dal�, Pediatrik Endokrinoloji B�l�m�, �i�li Hamidiye Etfal E�itim ve Ara�t�rma Hastanesi, �stanbul, T�rkiye

Ama�: Santral puberte prekoks (SPP), yava� ilerleyen SPP (Y�-SPP) veya h�zl� ilerleyen SPP (H�-SPP) �eklinde seyredebilir. �lerleme h�z�, tedavi kararlar�n� belirlemede kritik �neme sahiptir. Bu �al��ma, tedavi alan ve almayan hastalar�n klinik verilerini kar��la�t�rmay� ve H�-SPP olgular�nda ilerlemeyi etkileyebilecek fakt�rleri belirlemeyi ama�lamaktad�r.
Gere� ve Y�ntem: Bu tek merkezli retrospektif g�zlemsel �al��maya, 2021-2023 y�llar� aras�nda �ocuk endokrinoloji klini�inde SPP nedeniyle takip edilen, ya�lar� 5-8 aras�nda de�i�en 406 k�z hasta dahil edilmi�tir. Hastalar, gonadotropin salg�lat�c� hormon agonisti (GnRHa) tedavisi almayan Y�-SPP grubuna (n=252) ve GnRHa tedavisi alan H�-SPP grubuna (n=154) ayr�lm��t�r. Hastalar, klinik, laboratuvar ve radyolojik bulgular�na g�re analiz edilmi�tir.
Bulgular: Puberte belirtilerinin ba�lad�� median ya� Y�-SPP grubu i�in 7.2 y�l (5-8 ya� aral��nda), H�-SPP grubu i�in 7 y�l (5-8 ya� aral��nda) olarak bulunmu�tur (p=0.352). Tek de�i�kenli analizde Tanner telar� evresi, Luteinizan hormon (LH), Follik�l stim�le edici hormon (FSH), �stradiol, Pik LH d�zeyleri ve kemik ya��/kronolojik ya� oranlar� H�-SPP grubunda anlaml� derecede daha y�ksek seyredildi. �ok de�i�kenli analizde Tanner telar� evresi (p=0.001) ve kemik ya��/kronolojik ya� oran� (p<0.001) ba��ms�z de�i�ken fakt�rler olarak �ne ��karken di�er parametrelerin anlaml�l��n� yitirdi�i g�r�ld� (p>0.05).
Sonu�: Bu �al��mada, kemik ya��/kronolojik ya� oran�n�n, h�zl� ilerleyen puberte prekoks olgular�n�n erken tan�s�nda �nemli bir parametre oldu�u belirlenmi�tir. Puberte prekoks olgular�n� s�n�fland�rmak i�in klinik, laboratuvar ve radyolojik bulgular�n birlikte de�erlendirilmesi ve tedavi kararlar�n�n bireysel de�erlendirmelere dayand�r�lmas� kritik �neme sahiptir.

Anahtar Kelimeler: GnRHa tedavisi, Kemik ya��, Kronolojik ya�, Puberte prekoks

Comparative Analysis Of Girls With Slowly Progressive Central Precocious Puberty Vs. Rapidly Progressive Central Precocious Puberty: Single-Center Experience

B�sra Tetik Dincer¹, Aydilek Dagdeviren Cak�r², Ahmet Ucar²
¹Department of Pediatrics, Dr. Sami Ulus Children's Health and Diseases Training and Research Hospital, Ankara, Turkiye
²Department of Pediatrics, Division of Pediatric Endocrinology, Sisli Hamidiye Etfal Training and Research Hospital, Istanbul, Turkiye

Objectives: Central precocious puberty (CPP) can present as either slowly progressing CPP (SP-CPP) or rapidly progressing CPP (RP-CPP). The speed of progression is critical in determining treatment decisions. This study aims to compare the clinical data between patients who received treatment and those who did not, and to identify factors that may influence the progression in cases of RP-CPP.
Methods: This single-center retrospective observational study includes 406 female patients aged 5-8 years who were followed for CPP at the pediatric endocrinology clinic between 2021 and 2023. The patients were categorized into two groups: those with SP-CPP who did not receive gonadotropin-releasing hormone agonist (GnRHa) treatment (n=252) and those with RP-CPP who did receive GnRHa treatment (n=154). Patients were analyzed according to clinical, laboratory, and radiological findings.
Results: The median age at onset of pubertal signs were 7.2 years (Range 5-8) for the SP-CPP group and 7 (5-8) years for the RP-CPP group (p=0.352). In univariate analysis, Tanner breast stage, luteinizing hormone (LH), follicle-stimulating hormone (FSH), estradiol, peak LH levels, and bone age/chronological age ratios were significantly higher in the RP-CPP group. In multivariate logistic regression analysis, Tanner breast stage (p=0.001) and the bone age/chronological age ratio (p<0.001) were found to be a significant parameter, while other variables were not significant (p>0.05).
Conclusion: In this cohort, the bone age/chronological age ratio is a significant parameter for early detection of rapidly progressing precocious puberty cases. It is crucial to classify early puberty cases by evaluating clinical, laboratory, and radiological findings collectively and to make treatment decisions based on individual assessments.

Keywords: Bone age, Chronological age, GnRHa treatment, Precocious puberty

Sorumlu Yazar: B�sra Tetik Dincer
Makale Dili: �ngilizce

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