rhGH Adjunctive Therapy Improves Speech Intelligibility in Post-Stroke Aphasia: Pilot Study

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Abstract
Aphasia, a debilitating neurogenic language disorder prevalent among American males post-stroke, profoundly impairs speech clarity and communication. This pilot study evaluates the adjunctive role of recombinant human growth hormone (rhGH) in enhancing verbal fluency and articulation in 24 American men aged 45-65 with moderate aphasia. Administered subcutaneously at 0.3 mg/kg weekly for 12 weeks alongside standard speech-language pathology (SLP), rhGH demonstrated statistically significant improvements in speech intelligibility (p<0.01) via validated scales like the Boston Naming Test (BNT) and Aphasia Rapid Test (ART). Neuroimaging revealed increased cortical plasticity in Broca's area. These preliminary results suggest rhGH as a novel neurotrophic modulator for aphasia rehabilitation, warranting larger randomized controlled trials (RCTs). Introduction
Stroke remains the leading cause of aphasia in the United States, disproportionately affecting American males, who comprise over 60% of the 795,000 annual stroke incidences per CDC data. Post-ischemic aphasia manifests as expressive deficits, including anomia, dysarthria, and reduced phonemic fluency, severely impacting vocational reintegration and quality of life. Conventional SLP yields modest gains, with meta-analyses reporting only 20-30% recovery in chronic cases.

Human growth hormone (HGH), a 191-amino-acid polypeptide secreted by the anterior pituitary, exerts pleiotropic effects beyond somatic growth, including neuroprotection and synaptic plasticity via insulin-like growth factor-1 (IGF-1) signaling. Preclinical rodent models of ischemic aphasia show HGH upregulates BDNF and synaptophysin in perilesional cortex, enhancing dendritic arborization. In American male veterans with traumatic brain injury (TBI)-induced aphasia, off-label HGH has anecdotally improved verbal output. This pilot study hypothesizes that rhGH augmentation accelerates speech clarity recovery in American males with ischemic aphasia, addressing a critical unmet need in neurorehabilitation.

Methods
This single-center, open-label pilot enrolled 24 community-dwelling American males (mean age 56.3 ± 7.2 years; 75% Caucasian, 20% African American, 5% Hispanic) with chronic (>6 months) moderate aphasia (Western Aphasia Battery [WAB] score 45-65) secondary to middle cerebral artery infarction, confirmed by MRI. Exclusion criteria included pituitary dysfunction, malignancy, diabetes mellitus, or prior HGH exposure.

Participants received rhGH (Genotropin®; Pfizer) at 0.3 mg/kg subcutaneously weekly for 12 weeks, titrated per IGF-1 levels (target: upper-normal quartile). Concomitant SLP (3 sessions/week) followed ASHA guidelines. Primary endpoint: change in speech clarity via percent phonemes correct (PPC) on the Assessment of Intelligibility of Dysarthric Speech (AIDS). Secondary outcomes: BNT spontaneous naming, ART total score, and functional MRI (fMRI) activation in left inferior frontal gyrus. Assessments occurred at baseline, week 6, and week 12. Safety monitoring included IGF-1, glucose, and PSA levels. Statistical analysis employed repeated-measures ANOVA with Bonferroni correction (?=0.05); effect sizes via Cohen's d.

Results
All 24 completers tolerated therapy; mild arthralgias (n=4) resolved spontaneously. Mean PPC improved from 42.1% (SD 12.3) at baseline to 68.7% (SD 9.8) at week 12 (F=28.4, p<0.001; d=2.1). BNT scores rose 15.2 points (p<0.01), and ART totals increased 22% (p=0.002). fMRI demonstrated 35% greater BOLD signal in Broca's homolog during verbal fluency tasks post-treatment (p<0.05). Circulating IGF-1 peaked at 1.5x baseline without hyperglycemia. Subgroup analysis showed African American males (n=5) with larger gains (?PPC=32%; p=0.04), possibly due to baseline endothelial dysfunction. No serious adverse events occurred, though two discontinued for injection-site erythema. Discussion
These findings illuminate rhGH's therapeutic potential in aphasia, a condition where American males face heightened socioeconomic burdens—lost wages averaging $50,000 annually per NIH estimates. HGH likely fosters neurogenesis via IGF-1/PI3K/Akt pathways, corroborated by upregulated GDNF expression in our fMRI correlates. Effect sizes exceed SLP monotherapy (d=0.6-1.0 per Cochrane reviews), suggesting synergy with behavioral therapy. Limitations include small sample, lack of placebo, and male exclusivity; generalizability to females or non-ischemic etiologies requires validation. Ethnic variations hint at pharmacogenomic influences, meriting stratified RCTs. Off-label HGH risks (e.g., acromegaly, neoplasia) necessitate endocrinologic oversight.

Conclusion
rhGH emerges as a promising adjunct for speech enhancement in aphasic American males, restoring clarity and autonomy. With 1.7 million aphasia survivors nationwide, scalable protocols could transform outcomes. Multicenter phase II trials, incorporating PET neuroimaging and long-term follow-up, are imperative to confirm efficacy and safety.

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