Abstract
Isolated growth hormone deficiency Type II (IGHD II) is a rare autosomal dominant disorder caused by heterozygous GH1 gene mutations. Recombinant human GH (rhGH) has long been the standard therapy, but long-term real-world data on long-acting GH (LAGH) in patients with IGHD II are limited. The coexistence of IGHD II with Chiari malformation type 1 (CM1) presents additional clinical challenges. We report an 8-year follow-up of a male patient diagnosed at 4 years 3 months with severe short stature (80.2 cm, -6.43 standard deviation score [SDS]). Endocrine evaluation revealed profound GH deficiency (peak GH 0.23 ng/mL) and markedly low insulin-like growth factor-1 (IGF-1) (<25 ng/mL). Magnetic resonance imaging showed pituitary hypoplasia (height 1 mm) and suspected CM1. Genetic sequencing identified a previously classified pathogenic, de novo heterozygous splice site mutation in GH1 intron 3 (c.291+1G>A). However, his cognitive evaluation indicated significant impairment at age 12 years. Initiation of weekly LAGH at 4.2 years resulted in rapid catch-up growth (height SDS +2.75 in the first year) and sustained normalization of IGF-1. The therapy was well tolerated over 8 years, with no adverse events or radiological progression of CM1. This is the first and longest reported real-world follow-up of weekly LAGH in a genetically confirmed IGHD II patient with CM1, supporting its safety and efficacy. The patient's cognitive impairment prompts reflection on the possibility that earlier detection and treatment might contribute to improved intellectual outcomes. This represents the longest real-world follow-up of weekly LAGH in genetically confirmed IGHD II complicated by CM1.