Phosphatase and tensin homolog deleted on chromosome 10 (PTEN) is a well-known tumor suppressor whose mutation induces a variety of cancers in human. By dephosphorylating the D3 position of PIP3 (phosphatidylinositol-3,4,5- triphosphate), PTEN functions as a negative regulator to reduce PIP3, a signaling molecule for polarized cell migration in cellular level studies. However, the role of PTEN in cellular migration in organism has been difficult to study. In this regards, the study of PTEN in embryogenesis is a step further toward the understanding of PTEN in organismal level. Here, I used zebrafish as a model to investigate the role of PTEN in embryogenesis, in particular during gastrulation. I demonstrated that PTENB, one of the PTEN isoforms, regulates convergence and extension during zebrafish gastrulation. Knocking down ptenb by antisense morpholino oligonucleotide interfered with normal dorsoventral morphogenesis without perturbing dorsoventral patterning. The defects could be rescued by inhibiting PI3-kinase which demonstrated that ptenb may affect the process through controlling the PIP2/PIP3 balance. At the cellular level, the ptenb knockdown affects polarity and persistency of lamellapodia of lateral convergent cells. Furthermore, actin polymerization was increased in the ptenb-knockdown embryos. These results correlate to the PTEN study in culture cells to show that PTEN acts via the PIP3-, Rac 1- and Cdc42-dependent signaling pathway. Therefore, in this work I not only first confirm this pathway in an animal study but reveal the convergence and extension in zebrafish require ptenb to control the balance of PIP3 and PIP2 for normal cell migrating behaviors.