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Three Pairs of Protease-Serpin Complexes Cooperatively Regulate the Insect Innate Immune Responses
Authors:Rui Jiang  Eun-Hye Kim  Ji-Hee Gong  Hyun-Mi Kwon  Chan-Hee Kim  Kyoung-Hwa Ryu  Ji-Won Park  Kenji Kurokawa  Jinghai Zhang  David Gubb  and Bok-Luel Lee
Institution:From the National Research Laboratory of Defense Proteins, College of Pharmacy, Pusan National University, Busan 609-735, Korea, ;the §School of Life Science and Biopharmaceutics, Shenyang Pharmaceutical University, Shenyang 110016, China, and ;the Functional Genomics Unit, CIC bioGUNE, 48160 Derio, Spain
Abstract:Serpins are known to be necessary for the regulation of several serine protease cascades. However, the mechanisms of how serpins regulate the innate immune responses of invertebrates are not well understood due to the uncertainty of the identity of the serine proteases targeted by the serpins. We recently reported the molecular activation mechanisms of three serine protease-mediated Toll and melanin synthesis cascades in a large beetle, Tenebrio molitor. Here, we purified three novel serpins (SPN40, SPN55, and SPN48) from the hemolymph of T. molitor. These serpins made specific serpin-serine protease pairs with three Toll cascade-activating serine proteases, such as modular serine protease, Spätzle-processing enzyme-activating enzyme, and Spätzle-processing enzyme and cooperatively blocked the Toll signaling cascade and β-1,3-glucan-mediated melanin biosynthesis. Also, the levels of SPN40 and SPN55 were dramatically increased in vivo by the injection of a Toll ligand, processed Spätzle, into Tenebrio larvae. This increase in SPN40 and SPN55 levels indicates that these serpins function as inducible negative feedback inhibitors. Unexpectedly, SPN55 and SPN48 were cleaved at Tyr and Glu residues in reactive center loops, respectively, despite being targeted by trypsin-like Spätzle-processing enzyme-activating enzyme and Spätzle-processing enzyme. These cleavage patterns are also highly similar to those of unusual mammalian serpins involved in blood coagulation and blood pressure regulation, and they may contribute to highly specific and timely inactivation of detrimental serine proteases during innate immune responses. Taken together, these results demonstrate the specific regulatory evidences of innate immune responses by three novel serpins.
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