Yes-associated protein (YAP, 65Kd) is characterized as a key element of their functions in Hippo signal transduction pathway. However, the characterization of the proteins which interact with it is also required in order to elucidate further the biological role of YAP. TAZ (transcriptional coactivator) has also attracted considerable attention in the past decade, owing to its central role in the Hippo pathway. YAP and TAZ have robust and diverse biological functions, such as cell contact inhibition, mechanotransduction, differentiation, proliferation, and tumorigenesis. Recent explorations have revealed the interplay between YAP/TAZ and metabolism. Others documented that several proteins interactions with YAP/TAZ also profoundly promote their cytoplasmic or nuclear retention. They suggested that the protein COOH-terminal PDZ-binding motif plays a role in the regulation of YAP. Its deletion induces YAP re-localization to the cytoplasm and inhibits its activity. Zonula Occludens (ZO)-2 interacts with YAP in a PDZ-dependent manner and co-localizes with YAP into the nucleus. In this review we discuss the recent discoveries of YAP/TAZ roles in Hippo signaling with Tip60.