Fluticasone Propionate Orally Disintegrating Tablet (APT-1011) for Eosinophilic Esophagitis: Randomized Controlled Trial.

Topical steroids are effective treatments for eosinophilic esophagitis (EoE). The FLUTE (Fluticasone in EoE) trial evaluated safety and efficacy of APT-1011 (fluticasone propionate oral disintegrating tablet) vs placebo for treatment of EoE. In this randomized, double-blind, placebo-controlled, dose-finding, phase 2b trial, 106 adults with EoE received 1 of 4 APT-1011 doses or placebo for a 12-week induction period and 40 weeks of maintenance. Primary outcome was histologic response (≤6 eosinophils per high-power field) at Week 12. Secondary outcomes included endoscopic features and dysphagia frequency. Histologic response rates were 0% for placebo, 80% for APT-1011 3 mg twice daily (BID), 67% for 3 mg at bedtime (HS), 86% for 1.5 mg BID, 48% for 1.5 mg HS (P < .001 for all groups vs placebo). At Week 12, mean Edema/Rings/Exudates/Furrows/Strictures (EoE Endoscopic Reference Score) total score (max, 9.0) improved from 4.5 to 2.3 for 3 mg BID, 5.3 to 2.1 for 3 mg HS, 4.6 to 1.7 for 1.5 mg BID, 5.3 to 2.9 for 1.5 mg HS vs 5.2 to 4.5 for placebo. Mean dysphagia frequency over 14 days improved from baseline to Week 12 with all active groups improving more than placebo. Improvements were sustained to Week 52. APT-1011 was safe and well-tolerated, with higher incidence of candidiasis noted at the higher twice daily doses. APT-1011 dosing regimens were superior for histologic and endoscopic responses, and for reduction in dysphagia frequency vs placebo. Based on the symptom improvement and assessment of adverse events together with the histologic response rate, 3 mg once daily at bedtime dose showed the most favorable risk-benefit profile. gov, Number: NCT03191864

Boolean like algebras

Using Vaggione’s concept of central element in a double pointed algebra, we introduce the notion of Boolean like variety as a generalization of Boolean algebras to an arbitrary similarity type. Appropriately relaxing the requirement that every element be central in any member of the variety, we obtain the more general class of semi-Boolean like varieties, which still retain many of the pleasing properties of Boolean algebras. We prove that a double pointed variety is discriminator i↵ it is semi-Boolean like, idempotent, and 0-regular. This theorem yields a new Maltsev-style characterization of double pointed discriminator varieties. Moreover, we show that every idempotent semi-Boolean-like variety is term equivalent to a variety of noncommutative Boolean algebras with additional regular operations

Deletion Without Rebalancing in Multiway Search Trees

Many database systems that use a B + tree as the underlying data structure do not do rebalancing on deletion. This means that a bad sequence of deletions can create a very unbalanced tree. Yet such databases perform well in practice. Avoidance of rebalancing on deletion has been justified empirically and by average-case analysis, but to our knowledge no worst-case analysis has been done. We do such an analysis. We show that the tree height remains logarithmic in the number of insertions, independent of the number of deletions. Furthermore the amortized time for an insertion or deletion, excluding the search time, is O(1), and nodes are modified by insertions and deletions with a frequency that is exponentially small in their height. The latter results do not hold for standard B + trees. By adding periodic rebuilding of the tree, we obtain a data structure that is theoretically superior to standard B + trees in many ways. We conclude that rebalancing on deletion can be considered harmful

Effect of PF-00547659 on central nervous system immune surveillance and circulating β7+ T cells in Crohn's disease: Report of the TOSCA study

Background and Aims: Progressive multifocal leukoencephalopathy [PML], a brain infection associated with anti-integrin drugs that inhibit lymphocyte translocation from bloodstream to tissue, can be fatal. Decreased central nervous system [CNS] immune surveillance leading to this infection has been reported in patients with multiple sclerosis or Crohn's disease treated with antiintegrin antibody natalizumab. PF-00547659 is an investigational human monoclonal antibody for inflammatory bowel disease, targeted against α4β7-mucosal addressin cell-adhesion molecule-1 [the integrin ligand selectively expressed in the gut]. We hypothesised that this selective agent would not affect central nervous system immune surveillance. Methods: Cerebrospinal fluid from five healthy volunteers, and from 10 patients with Crohn's disease previously treated with immunosuppressants, was evaluated to assess the feasibility of the study. Subsequently, 39 patients with active Crohn's disease and previous immunosuppression were evaluated over 12 weeks of PF-00547659-induction therapy. We measured total lymphocytes, T cell subsets in cerebrospinal fluid, and circulating β7+ memory cells. Disease activity was assessed using the Harvey-Bradshaw Index. Results: Patients treated with PF-00547659 had no reduction of cerebrospinal fluid lymphocytes, T-lymphocyte subsets, or CD4:CD8 ratio, whereas circulating β7+ memory cells increased significantly. A total of 28/35 [80%] patients had a clinical response and 27/34 [79%] had disease remission. Treatment-related adverse events, none serious, were reported in 23/49 [47%] patients. Conclusions: In patients with active Crohn's disease, natalizumab therapy increases the risk for PML, and the increased risk is thought to be associated with iatrogenic leukopenia within the CNS. PML under PF-00547659 may be a lesser concern, as this agent did not reduce lymphocytes or T cell subsets in the cerebrospinal fluid.SCOPUS: ar.jinfo:eu-repo/semantics/publishe