ABSTRACT
The anaerobic ammonium oxidation (anammox) process is widely used for N-rich wastewater treatment. In the current research the deammonification reactor in a reverse order (first anammox, then the nitrifying biofilm cultivation) was started up with a high maximum N removal rate (1.4 g N m(-2) d(-1)) in a moving bed biofilm reactor. Cultivated biofilm total nitrogen removal rates were accelerated the most by anammox intermediate - nitric oxide (optimum 58 mg NO-N L(-1)) addition. Furthermore, NO was added in order to eliminate inhibition caused by nitrite concentrations (>50 mg [Formula: see text]) increasing [Formula: see text] (2/1, respectively) along with a higher ratio of [Formula: see text] (0.6/1, respectively) than stoichiometrical for this optimal NO amount added during batch tests. Planctomycetales clone P4 sequences, which was the closest (98% and 99% similarity, respectively) relative to Candidatus Brocadia fulgida sequences quantities increase to 1 × 10(6) anammox gene copies g(-1) total suspended solids to till day 650 were determined by quantitative polymerase chain reaction.
Subject(s)
Ammonium Compounds/metabolism , Biofilms , Nitric Oxide/metabolism , Nitrites/metabolism , Planctomycetales/physiology , Anaerobiosis , Bioreactors , Oxidation-ReductionABSTRACT
Trypanosoma cruzi trans-sialidase (TS) was identified three decades ago. TS catalyses a trans-glycosylation reaction, transferring SA from sialylated donors to the terminal galactose mucin-glycoconjugates, or non-mucin galactyosyl-glycoconjugates. It is an external surface protein that is also released from the parasite, displaying several binding properties in addition to its enzymatic function. TS structure has been solved and its catalytic properties are well known, providing tools for development of new inhibitors, as potential chemotherapeutic agents against Chagas' disease. However, there are still several unsolved questions regarding TS role in the biology of T. cruzi and in the pathology of Chagas' disease. In this review, we will describe the multifunctional roles of TS regarding the development of Chagas' disease and propose that these multiple functions have to be considered in future investigations aiming to use TS as a drug target.
