Growth hormone deficiency risk factors

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief:

Overview

Risk Factors

Genetics

POU1F1 gene mutations

• It is the most common known genetic cause of the combined pituitary hormone deficiency.^[4]
• It is responsible for pituitary-specific transcription of genes for GH, prolactin, thyrotropin, and the growth hormone-releasing hormone (GHRH) receptor.^[5]
• PROP1 mutations result in failure to activate POU1F1/Pit1 gene expression and probably cause pituitary hypoplasia.^[6]

GH1 gene mutations

• It is GH1 is the gene encoding GH, located on chromosome 17.
• Gene deletions, frameshift mutations, and nonsense mutations of GH1 have been described as causes of familial GHD.

Syndrome of bioinactive GH

• Bioinactive GH has the main symptoms and signs of isolated GHD with normal basal GH levels and low insulin-like growth factor I concentrations.^[7]

GH receptor signal transduction

• It is essential for normal signaling of the GH receptor. Mutations in the gene encoding signal transducer decrease the response of receptors to GH.^[8]

IGF-I gene mutations

• Mutations in the gene encoding IGF-I cause a unique syndrome of GHD.^[9]
• Patients with IGF-I gene mutations have prenatal growth failure, microcephaly, significant neurocognitive deficits, and sensorineural hearing loss.

Defective stabilization of circulating IGF-I

• Acid-labile subunit is important for the stabilization of the IGF-I.
• Mutations in the gene coding for it causes less stable and subsequently less effect.^[10]

IGF-I receptor mutations

• Mutations in the gene encoding the receptor for the IGF-I result in partial loss of function of the IGF-I receptor.^[11]

References

Template:WH Template:WS