Recent data indicate that TGF beta3, one member of the TGF beta -isoforms,
has an important role in bone remodeling. Up to date little is known about
the expression and regulation of TGF beta3 in man. We established a highly
specific ELISA for quantitative measurement of TGF beta3 in bone and blood
samples and a RT-PCR in combination with HPLC for detection and quantificat
ion of TGF beta3 mRNA in 89 human bone samples. Levels of TGF beta3 protein
ranged between 30 and 66 pg/mg bone (mean 36,6 +/- 1,03 pg/mg) and between
30 and 1910 pg/ml in serum (mean 128,9 +/- 35.9 pg/ml). TGFB3 mRNA express
ion as well as protein levels in serum and in bone declined age dependently
. No specific load- or site-specific distribution of TGF beta3 mRNA express
ion or protein content was detected at different sites indicating an absenc
e of mechanical regulation. Protein levels of TGF beta3 in serum correlated
with TGFB3 mRNA expression in bone (p= 0.0027; r=0.49). By contrast, TGF b
eta3 protein levels stored in the bone matrix were not related to TGF beta3
mRNA reflecting the long term process of TGF beta3 deposition during bone
remodeling. Notably TGF beta3 serum levels were highly correlated with IGF-
Id and osteocalcin levels in serum. We conclude that TGF beta3 in man circu
lates in significant amounts which appears to be representative for TGF bet
a3 expression in bone tissue and may be in part derived from bone. The high
correlation of TGFB3 with IGF-I suggests parallel systemic principles of r
egulation.