Obesity is implicated as a risk factor in 6 out of the 10 major causes of death, namely malignant tumour , heart disease , brain blood vessel disease , diabetes , chronic liver diseases, cirrhosis and hypertension. Hedgehog (Hh) signaling is known as a pivotal regulator during invertebrate and vertebrate embryonic development, and is known to cause various tumors if it is hyperactivated beyond normal status. However, whether Hedgehog signaling is involved in fat formation is not defined clearly . Hence, this project aimed to elucidate the effect of Hh in adipogenesis. 3T3-L1 cell and mouse adipogenesis models are used to assay the Hh signaling during the entire process. Our data showed that Hh signaling was decreased during adipogenesis. Hh signaling was also compared between failed adipogenesis and successful adipogenesis. The results showed that only in successfully differentiated adipocytes that Hh _expression was downregulated. Furthermore, comparable effects of Hh in fat formation was seen in mice. We conclude that Hh signaling inhibits fat formation under both in vivo and in vitro conditions. Results of this study potentiate the use of Hh pathway in developing therapeutic targets for obesity and in prevention of diseases caused by obesity.