Heterologous biosynthesis and manipulation of crocetin in Saccharomyces cerevisiae

Background: Due to excellent performance in antitumor, antioxidation, antihypertension, antiatherosclerotic and antidepressant activities, crocetin, naturally exists in Crocus sativus L., has great potential applications in medical and food fields. Microbial production of crocetin has received increasing concern in recent years. However, only a patent from EVOVA Inc. and a report from Lou et al. have illustrated the feasibility of microbial biosynthesis of crocetin, but there was no specific titer data reported so far. Saccharomyces cerevisiae is generally regarded as food safety and productive host, and manipulation of key enzymes is critical to balance metabolic flux, consequently improve output. Therefore, to promote crocetin production in S. cerevisiae, all the key enzymes, such as CrtZ, CCD and ALD should be engineered combinatorially. Results: By introduction of heterologous CrtZ and CCD in existing a-carotene producing strain, crocetin biosynthesis was achieved successfully in S. cerevisiae. Compared to culturing at 30 degrees C, the crocetin production was improved to 223 mu g/L at 20 degrees C. Moreover, an optimal CrtZ/CCD combination and a titer of 351 mu g/L crocetin were obtained by combinatorial screening of CrtZs from nine species and four CCDs from Crocus. Then through screening of heterologous ALDs from Bixa orellana (Bix_ ALD) and Synechocystis sp. PCC6803 (Syn_ ALD) as well as endogenous ALD6, the crocetin titer was further enhanced by 1.8-folds after incorporating Syn_ ALD. Finally a highest reported titer of 1219 mu g/L at shake flask level was achieved by overexpression of CCD2 and Syn_ ALD. Eventually, through fed-batch fermentation, the production of crocetin in 5-L bioreactor reached to 6278 mu g/L, which is the highest crocetin titer reported in eukaryotic cell. Conclusions: Saccharomyces cerevisiae was engineered to achieve crocetin production in this study. Through combinatorial manipulation of three key enzymes CrtZ, CCD and ALD in terms of screening enzymes sources and regulating protein expression level (reaction temperature and copy number), crocetin titer was stepwise improved by 129.4fold (from 9.42 to 1219 mu g/L) as compared to the starting strain. The highest crocetin titer (6278 mu g/L) reported in microbes was achieved in 5-L bioreactors. This study provides a good insight into key enzyme manipulation involved in serial reactions for microbial overproduction of desired compounds with complex structure.