| Abstract | dc.description.abstract | Purpose Recent reports discuss the altered bone homeostasis
in cigarette smokers, being a risk factor for osteoporosis
and negatively influencing fracture healing. Cigarette smoke
is known to induce oxidative stress in the body via an
increased production of reactive oxygen species (ROS).
These increases in ROS are thought to damage the boneforming
osteoblasts. Naturally occurring polyphenols
contained in green tea extract (GTE), e.g., catechins, are
known to have anti-oxidative properties. Therefore, the aim
of this study was to investigate whether GTE and especially
catechins protect primary human osteoblasts from cigarette
smoke-induced damage and to identify the underlying
mechanisms.
Methods Primary human osteoblasts were isolated from
patients’ femur heads. Cigarette smoke medium (CSM)
was obtained using a gas-washing bottle and standardized
by its optical density (OD320) at λ0320 nm. ROS formation
was measured using 2′7′dichlorofluorescein diacetate, and
osteoblasts’ viability was detected by resazurin conversion.
Results Co-, pre-, and post-incubation with GTE and
catechins significantly reduced ROS formation and thus
improved the viability of CSM-treated osteoblasts.
Besides GTE’s direct radical scavenging properties,
pre-incubation with both GTE and catechins protected
osteoblasts from CSM-induced damage. Inhibition of the
anti-oxidative enzyme HO-1 significantly reduced the
protective effect of GTE and catechins emphasizing the
key role of this enzyme in GTE anti-oxidative effect.
Conclusions Our data suggest possible beneficial effects on
bone homeostasis, fracture healing, and bone mineral density
following a GTE-rich diet or supplementation. | es_CL |
