Anti-programmed death 1 (PD-1) immune checkpoint inhibitors enhance the antitumour activity of the immune system and have produced durable tumour responses in several solid tumours including non-small cell lung cancer (NSCLC). However, PD-1 inhibitors can lead to immune-related adverse events , including pneumonitis, which is typically mild, but can be severe and potentially fatal. Pneumonitis often resolves with steroids, but some cases are steroid refractory, leading to a relapsing and remitting course in milder cases or the need for salvage therapies in more severe cases. Here, we present two patients with NSCLC who developed severe pneumonitis following therapy with nivolumab and pembrolizumab. While one patient improved with steroids and infliximab, the other patient failed to respond to steroids and subsequently died. These cases demonstrate the highly variable presentation and therapeutic responses seen in patients with pneumonitis following anti-PD-1 therapy and illustrate that severe cases can often present refractory to steroid therapy.
Background: Chitin synthases are stimulated by N-acetylglucosamine (GlcNAc).Results: GlcNAc and 2-acylamido analogues of GlcNAc stimulate formation of chitin oligosaccharides by yeast chitin synthase, and GlcNAc is transferred to the 2-acylamido analogues.Conclusion: Chitin synthases use GlcNAc analogues as primers and transfer one GlcNAc at a time.Significance: Results are new insights into polysaccharide synthase mechanism and suggest ways of synthesizing novel modified polysaccharides.
The novel severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) was declared a pandemic by the WHO in March 2020. As of August 2021, more than 220 countries have been affected, accounting for 211,844,613 confirmed cases and 4,432,802 deaths worldwide. A new delta variant wave is sweeping through the globe. While previous reports consistently have demonstrated worse prognoses for patients with existing cardiovascular disease than for those without, new studies are showing a possible link between SARS-CoV-2 infection and an increased incidence of new-onset heart disease and diabetes, regardless of disease severity. If this trend is true, with hundreds of millions infected, the disease burden could portend a potentially troubling increase in heart disease and diabetes in the future. Focusing on heart failure in this review, we discuss the current data at the intersection of COVID, heart failure, and diabetes, from clinical findings to potential mechanisms of how SARS-CoV-2 infection could increase the incidence of those pathologies. Additionally, we posit questions for future research areas regarding the significance for patient care.
Inorganic polyphosphates, linear
polymers of orthophosphate, occur
naturally throughout biology and have many industrial applications.
Their biodegradable nature makes them attractive for a multitude of
uses, and it would be important to understand how polyphosphates are
turned over enzymatically. Studies of inorganic polyphosphatases are,
however, hampered by the lack of high-throughput methods for detecting
and quantifying rates of polyphosphate degradation. We now report
chromogenic and fluorogenic polyphosphate substrates that permit spectrophotometric
monitoring of polyphosphate hydrolysis and allow for high-throughput
analyses of both endopolyphosphatase and exopolyphosphatase activities,
depending on assay configuration. These substrates contain 4-nitrophenol
or 4-methylumbelliferone moieties that are covalently attached to
the terminal phosphates of polyphosphate via phosphoester linkages
formed during reactions mediated by EDAC (1-ethyl-3-(3-(dimethylamino)propyl)carbodiimide).
This report identifies Nudt2 as an inorganic polyphosphatase and also
adds to the known coupling chemistry for polyphosphates, permitting
facile covalent linkage of alcohols with the terminal phosphates of
inorganic polyphosphate.
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