PDF Checkpoint 1.8.9
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It's true that the /spawnpoint command can be useful because you don't have to wait for the night to create a checkpoint, but sometimes you may want to have a BUD switch connected to the bed or something similar, so that you don't have to type the command in every time. To do this, you just need to have a discreet pressure plate connected to a block with the /time set 18000 command, and it will set the time to night so the player can sleep.
Basilea Pharmaceutica Ltd. (SIX: BSLN) provided a general corporate update today. The company does not expect a material impact on the timelines of ongoing or planned oncology studies with the FGFR kinase inhibitor derazantinib and the planned phase 2a biomarker driven study with its tumor checkpoint controller, lisavanbulin, due to the coronavirus pandemic. The impact on the ongoing ceftobiprole phase 3 study remains limited, with patient enrolment timelines potentially extended by up to a quarter.
Derazantinib is an investigational orally administered small-molecule FGFR kinase inhibitor with strong activity against FGFR1, 2, and 3.3 FGFR kinases are key drivers of cell proliferation, differentiation and migration. FGFR genetic aberrations, e.g. gene fusions, mutations or amplifications, have been identified as potentially important therapeutic targets for various cancers, including intrahepatic cholangiocarcinoma (iCCA), urothelial, breast, gastric and lung cancers.4 In these cancers, FGFR genetic aberrations are found in a range of 5% to 30%.5 Derazantinib also inhibits the colony-stimulating-factor-1-receptor kinase (CSF1R).3, 6 CSF1R-mediated signaling is important for the maintenance of tumor-promoting macrophages and therefore has been identified as a potential target for anti-cancer drugs.7 Pre-clinical data has shown that tumor macrophage depletion through CSF1R blockade renders tumors more responsive to T-cell checkpoint immunotherapy, including approaches targeting PD-L1/PD-1.8, 9 Derazantinib has demonstrated antitumor activity and a manageable safety profile in previous clinical studies, including a biomarker-driven phase 1/2 study in iCCA patients,10 and has received U.S. and EU orphan drug designation for iCCA. Basilea is currently conducting two clinical studies with derazantinib. The first study, FIDES-01, is a registrational phase 2 study in patients with inoperable or advanced iCCA. It comprises one cohort of patients with FGFR2 gene fusions and another cohort of patients with mutations or amplifications.11 The second study, FIDES-02, is a phase 1/2 study evaluating derazantinib alone and in combination with Roche's PD-L1-blocking immune-checkpoint inhibitor atezolizumab (Tecentriq®) in patients with advanced urothelial cancer, including metastatic, or recurrent surgically unresectable disease, expressing FGFR genetic aberrations.12 Basilea in-licensed derazantinib from ArQule Inc, a wholly-owned subsidiary of Merck & Co., Inc., Kenilworth, N.J., U.S.A.
Basilea's oncology drug candidate lisavanbulin,BAL101553, (the prodrug of BAL27862)13 is being developed as a potential therapy for diverse cancers.14, 15, 16 In pre-clinical studies, lisavanbulin demonstrated in-vitro and in-vivo activity against diverse treatment-resistant cancer models, including tumors refractory to conventional approved therapeutics and radiotherapy.17, 18, 19 Lisavanbulin efficiently distributes to the brain, with anticancer activity in glioblastoma models.20, 21, 22 In pre-clinical studies, end-binding protein 1 (EB1) was identified as a potential response-predictive biomarker in glioblastoma models.22 The active moiety BAL27862 binds to the colchicine site of tubulin, with distinct effects on microtubule organization,23 resulting in the activation of the "spindle assembly checkpoint" which promotes tumor cell death.24
For gastroenterologists and hepatologists, immunotherapy-related hepatotoxicity deserves special mention as it is commonly encountered. Furthermore, checkpoint inhibitors have recently been added to first- and second-line treatment options for advanced hepatocellular carcinoma (HCC) after promising clinical trial results[3-5]. These patients tend to have relatively limited liver reserve since most HCCs occur on a background of liver cirrhosis[6]. Thus, immunotherapy-related hepatotoxicity can result in liver failure and even death.
The logprocessor step is a chunk step that specifies batch artifacts for the reader (LogItemReader), the processor (LogItemProcessor), and the writer (LogItemWriter). This step creates a checkpoint for every ten items processed.
Specifies if processed items are buffered until it is time to take a checkpoint. If true, a single call to the item writer is made with a list of the buffered items before committing the chunk and taking a checkpoint.
This example defines a chunk step and specifies its reader, processor, and writer artifacts. The step updates a checkpoint and commits each chunk after processing five items. It skips all MyItemException exceptions and all its subtypes, except for MyItemSeriousSubException, up to a maximum of ten skipped exceptions. The step retries a chunk when a MyResourceTempUnavailable exception occurs, up to a maximum of three attempts.
This element specifies a batch artifact that sends intermediary results from each partition to a partition analyzer. The batch artifact sends the intermediary results after each checkpoint for chunk steps and at the end of the step for task steps. The batch artifact is an implementation of the PartitionCollector interface. 2b1af7f3a8