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PMID-20203154 – GLP-1RA Rodent Thyroid C-Cell Activation

PMID-20203154 – GLP-1RA Rodent Thyroid C-Cell Activation

Knudsen LB et al. "Glucagon-like peptide-1 receptor agonists activate rodent thyroid C-cells causing calcitonin release and C-cell proliferation," Endocrinology, 2010;151(4):1473-1486. doi:10.1210/en.2009-1272

Quick Reference

Property Value
PMID 20203154
DOI 10.1210/en.2009-1272
Year 2010
Journal Endocrinology
Study Type Animal in vivo
Evidence Level V
Sample Rodent models (rats and mice); primate (cynomolgus monkey) comparison
Peptide(s) Studied Semaglutide, Tirzepatide (GLP-1RA class)

Key Findings

  • GLP-1RAs (liraglutide, exenatide) caused dose-dependent thyroid C-cell proliferation in rodents
  • C-cell hyperplasia progressed to C-cell adenomas and medullary thyroid carcinoma (MTC) in rodents with chronic exposure
  • Calcitonin release was significantly elevated in rodent models
  • CRITICAL SPECIES DIFFERENCE: Primate thyroid C-cells showed NO proliferative response to GLP-1RAs
  • GLP-1 receptor expression is high in rodent thyroid C-cells but very low or absent in human/primate C-cells
  • This species-specific difference in GLP-1R expression explains the differential response
  • This study is the original basis for the FDA black-box warning on GLP-1RA labels regarding thyroid C-cell tumors

Study Design

Preclinical study combining in vivo rodent experiments (chronic dosing of GLP-1RAs with thyroid histopathology) with cross-species comparison using cynomolgus monkeys. Included dose-response analysis, calcitonin measurements, GLP-1R expression profiling by immunohistochemistry and RT-PCR across species, and long-term carcinogenicity assessment in rodents.

Limitations

  • Animal data; direct translation to human risk is uncertain
  • The rodent-specific finding has driven a black-box warning that may overstate human risk
  • Primate data limited to relatively short-term exposure
  • Doses used in rodent studies were often supraphysiological relative to clinical doses
  • The study does not address whether chronic human use at therapeutic doses produces any C-cell effects

Clinical Relevance

This is the foundational study behind the GLP-1RA thyroid cancer black-box warning. Understanding it is essential for patient counseling. The key message: rodent C-cell tumors were caused by species-specific GLP-1R expression that does not exist in humans. While the FDA appropriately required the warning based on preclinical data, the subsequent clinical evidence (PMID-41359966, PMID-38018310) shows that the actual human thyroid cancer risk is far lower than predicted from rodent data. Patients can be reassured that the black-box warning reflects regulatory caution from animal data, not confirmed human carcinogenicity. MTC/MEN2 family history remains a contraindication.

Related

#research #animal-in-vivo #evidence-level-V #cancer