TGF-beta Signaling in Development

doi:10.1126/stke.3992007cm1

Account Information

Guest Alerts | Access Rights | My Account | Sign In

Site Navigation

Article Views

Article Tools

Help & Feedback

My Science Signaling

Sci. STKE, 14 August 2007
Vol. 2007, Issue 399, p. cm1
[DOI: 10.1126/stke.3992007cm1]

CONNECTIONS MAP OVERVIEWS

TGF- $beta$ Signaling in Development

Krit Kitisin¹, Tapas Saha¹, Tiffany Blake¹, Nady Golestaneh¹, Merlyn Deng¹, Christine Kim¹, Yi Tang¹, Kirti Shetty¹, Bibhuti Mishra¹, and Lopa Mishra¹^,2^*

¹Laboratory of Cancer Genetics and Digestive Diseases, Department of Surgery, Department of Medicine, and Lombardi Comprehensive Cancer Center, Georgetown University, Washington, DC 20007, USA.
²Department of Veterans Affairs Medical Center, Washington, DC 20007, USA.

Abstract: The transforming growth factor– $beta$ (TGF- $beta$ ) superfamily comprises nearly 30 growth and differentiation factors that include TGF- $beta$ s, activins, inhibins, and bone morphogenetic proteins (BMPs). Multiple members of the TGF- $beta$ superfamily serve key roles in stem cell fate commitment. The various members of the family can exhibit disparate roles in regulating the biology of embryonic stem (ES) cells and tumor suppression. For example, TGF- $beta$ inhibits proliferation of multipotent hematopoietic progenitors, promotes lineage commitment of neural precursors, and suppresses epithelial tumors. BMPs block neural differentiation of mouse and human ES cells, contribute to self-renewal of mouse ES cells, and also suppress tumorigenesis. ES cells and tumors may be exposed to multiple TGF- $beta$ members, and it is likely that the combination of growth factors and cross-talk among the intracellular signaling pathways is what precisely defines stem cell fate commitment. This Connections Map Pathway in the Database of Cell Signaling integrates signaling not only from TGF- $beta$ and BMP but also from the ligands nodal and activin, and describes the role of the signaling pathways activated by these ligands in mammalian development. Much of the evidence for the connections shown comes from studies on mouse and human ES cells or mouse knockouts. This pathway is important for understanding not only stem cell biology, but also the molecular effectors of TGF- $beta$ and BMP signaling that may contribute to cancer suppression or progression and thus are potential targets for therapeutic intervention.

*Corresponding author. E-mail, lopamishra{at}yahoo.com

Citation: K. Kitisin, T. Saha, T. Blake, N. Golestaneh, M. Deng, C. Kim, Y. Tang, K. Shetty, B. Mishra, L. Mishra, TGF- $beta$ Signaling in Development. Sci. STKE 2007, cm1 (2007).

Read the Full Text

The editors suggest the following Related Resources on Science sites:

In Science Signaling

EDITORS' CHOICE
Structural Biology
Monogamy in the TGF-β Receptor Relationship: Nancy R. Gough (5 February 2008)
Sci. Signal. 1 (5), ec46. [DOI: 10.1126/stke.15ec46]
| Abstract »

THIS ARTICLE HAS BEEN CITED BY OTHER ARTICLES:

Crosstalk Between Vascular Endothelial Growth Factor, Notch, and Transforming Growth Factor-{beta} in Vascular Morphogenesis.: M. T. Holderfield and C. C.W. Hughes (2008)
Circ. Res. 102, 637-652
| Abstract » | Full Text » | PDF »

To Advertise | Find Products

Science Signaling. ISSN 1937-9145 (pre-2008: Science's STKE. ISSN 1525-8882)

You have reached the bottom of the page. Back to top

Site Tools

Site Search

Account Information