Publications by authors named "L J Ignarro"

Disappointing results from the POLAR A and M phase III trials involving colorectal cancer patients on chemotherapy with FOLFOX6 in curative (A) and palliative (M) settings have been reported by the principal investigators and the sponsor (PledPharma AB/Egetis Therapeutics AB). FOLFOX6, oxaliplatin in combination with 5-fluorouracil (5-FU), possesses superior tumoricidal activity in comparison to 5-FU alone, but suffers seriously from dose-limiting platinum-associated Chemotherapy-Induced Peripheral Neuropathy (CIPN). The aim of the POLAR trials was to demonstrate that PledOx [calmangafodipir; CaMn(DPDP)] reduced the incidence of persistent CIPN from 40% to 20%.

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On 2 July 2021, highly negative results were reported from the POLAR A and M phase III trials in patients with colorectal cancer, treated with an oxaliplatin-based regimen and co-treated with calmangafodipir (CaM; PledOx; PledPharma AB/Egetis Therapeutics AB) or placebo. The results revealed persistent chemotherapy-induced peripheral neuropathy (CIPN) in 54.8% of the patients treated with PledOx, compared with 40.

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Article Synopsis
  • - The report by Fan criticized the ProPerDP method for its ability to detect protein persulfidation, claiming it was inadequate based on their findings.
  • - Upon review, it was determined that Fan's claims were unsupported and stemmed from methodological flaws in their study.
  • - The authors assert that ProPerDP is still a trustworthy method for analyzing protein per/polysulfidation, as Fan's evaluations were based on unconfirmed assumptions.
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Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is characterized by massive inflammation of the arterial endothelium accompanied by vasoconstriction and widespread pulmonary micro thrombi. As a result, due to the destruction of nitric oxide (NO) by inflammatory superoxide (O), pulmonary NO concentration ceases, resulting in uncontrolled platelet aggregation and massive thrombosis, which kills the patients. Introducing NO by inhalation (INO) may replace the loss of endothelium-derived NO.

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