Protein tyrosine phosphatases (PTPs) are involved in the coordination of protein tyrosine kinases in various cellular processes. In Drosophila, many receptor-like protein tyrosine phosphatases(RPTPs), such as dLAR dPTP69D, and dPTP99A, are required for the development of neuromuscular junction (NMJ) but the role of non-transmembrane protein tyrosine phosphatases (NTPTPs) in NMJ development remains unknown. Recent studies have shown that one of Drosophila NTPTPs, dPTPmeg, is required for the axon projection establishment of the mushroom body. Here we studied the role of dPTPmeg in NMJ development. Gain-of-function analysis showed that dPTPmeg decreased the type Ib bouton numbers at Drosophila NMJ. However, dPTPmeg mutant does not cause obvious defects in NMJ development. We further identified Src as a dPTPmeg interacting protein. Drosophila Src has been shown to play a role in NMJ development. Genetic analysis revealed that Src knockdown could partially rescue dPTPmeg-induced NMJ defects. These findings suggest that Drosophila PTPmeg associate with Src in the regulation of NMJ development.