Acidic cellular environments: Activation of latent tgf-β and sensitization of cellular responses to tgf-β and egf

Regeneration involves a number of cellular processes: revascularisation, invasion by haemopoietic cells, removal of necrotic tissue and finally reformation of the tissues. These processes have been extensively studied in vitro and are known to be affected by various growth factors. However, it has p

Transforming growth factor␤1 (TGF␤1) elicits a multitude of cellular responses from the epithelial-derived human colon cancer Moser cells. TGF␤1 induces the expression of laminin and fibronectin, and previous studies show that the induction of fibronectin is functionally associated with the regulati

To clarify the role of transforming growth factor-b (TGF-b) and its receptors in hepatocyte growth, we studied the expression of TGF-b1 and its receptors and the sensitivity to growth inhibition by TGF-b1 protein in rat hepatocytes derived from resting and regenerating livers. In hepatocytes derived

Tat is a transcriptional transactivator produced by the human immunodeficiency virus type 1 (HIV-1) and plays a pivotal role in enhancing expression of the viral genome in the infected cells. Although initial studies have suggested that interaction of Tat with the transactivation responsive element

## Abstract Transforming growth factors β (TGF‐βs) are multifunctional cytokines, which are secreted in latent forms in large latent TGF‐β complexes (LL‐TGF‐β) with subsequent deposition to the extracellular matrix (ECM). While a variety of mechanisms capable of activating latent TGF‐β in vitro hav

A panel of 6 human glioma cell lines was examined for TGF-␤1 responsiveness. U-178 MG and U-251 MG AgCl1 were significantly inhibited by TGF-␤1, while U-343 MGa 31L and U-343 MGa 35L were potently stimulated to proliferate. TGF-␤1 induced endogenous PAI-1 protein synthesis, Smad binding element/(CAG