Adrenomedullin Therapy for Moderate-to-Severe COVID-19 Pneumonia: Double-Blind Placebo-Controlled Phase 2a Trial.

Publication date: Jul 14, 2025

Adrenomedullin (AM) is a bioactive peptide that is strongly induced during severe inflammation, including pneumonia and sepsis, and serves as an organ-protective factor. The plasma concentration of AM is markedly increased in the novel coronavirus disease COVID-19 and is closely related to the severity of the disease and prognosis of patients. We performed two investigator-initiated trials to evaluate the efficacy and safety of AM in patients with moderate-to-severe COVID-19. This multicenter, double-blind, placebo-controlled phase-2a trial evaluated COVID-19 patients with severe (n = 33) and moderate (n = 31) pneumonia in Japan. Patients were randomly assigned to receive either 15 ng/kg/min AM or placebo. The primary endpoint was the duration of mechanical ventilation (MV) for severe pneumonia and oxygen support for moderate pneumonia. The main secondary endpoint was clinical status up to 30 days after the intervention. No differences in primary or secondary endpoints were observed between the AM and placebo groups in patients with severe or moderate pneumonia. In the severe pneumonia group, three patients in the placebo group died due to respiratory failure, and one patient in the AM group died due to respiratory failure. The respiratory function test at 30 days in the moderate pneumonia group tended to be better than that in the AM group and approached significance (p = 0. 073). Although mild adverse events caused by the vasodilatory effects of AM were noted, the safety of AM for treating pneumonia was confirmed. In these trials, we did not observe a definitive efficacy of AM in moderate to severe pneumonia. Alternative strategies for the treatment of AM in pneumonia require further research.

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Concepts	Keywords
Blind	Adrenomedullin
Japan	Adrenomedullin
Plasma	adrenomedullin
Pneumonia	Adult
Therapy	Aged
	COVID-19
	COVID-19
	COVID-19 Drug Treatment
	Double-Blind Method
	Female
	Humans
	Japan
	Japanese
	Male
	mechanical ventilation
	Middle Aged
	pneumonia
	Respiration, Artificial
	SARS-CoV-2
	Treatment Outcome

Semantics

Type	Source	Name
disease	MESH	COVID-19
disease	MESH	Pneumonia
disease	MESH	inflammation
disease	MESH	sepsis
pathway	KEGG	Coronavirus disease
drug	DRUGBANK	Oxygen
disease	IDO	intervention
disease	MESH	respiratory failure
drug	DRUGBANK	Tropicamide
disease	MESH	Emergency
disease	MESH	Infectious Diseases
disease	MESH	critically ill
disease	MESH	lung injury
disease	MESH	renal failure
drug	DRUGBANK	Creatinine
disease	IDO	history
disease	MESH	malignancy
disease	MESH	abnormalities
disease	MESH	heart failure
disease	MESH	myocardial infarction
disease	IDO	symptom
disease	IDO	process
disease	MESH	death
drug	DRUGBANK	Carbon monoxide
drug	DRUGBANK	Alteplase
disease	IDO	assay
disease	IDO	blood
disease	MESH	clinical importance
disease	MESH	Complications
disease	MESH	Hypertension
disease	MESH	Pulmonary diffusing capacity
drug	DRUGBANK	Pentaerythritol tetranitrate
disease	MESH	Bacterial pneumonia
disease	MESH	Delirium
disease	MESH	Insomnia
disease	MESH	Bradycardia
disease	MESH	Aspiration pneumonia
disease	MESH	bleeding
disease	MESH	Thrombocytopenia
disease	IDO	infectivity
disease	MESH	viral pneumonia
disease	MESH	privacy
disease	IDO	production
disease	MESH	cardiovascular diseases
drug	DRUGBANK	Ferrous sulfate anhydrous
disease	IDO	endotoxin
disease	MESH	septic shock
disease	MESH	Hypotension
disease	MESH	shock
disease	MESH	pneumococcal pneumonia
drug	DRUGBANK	Diethylstilbestrol
disease	MESH	ulcerative colitis
disease	MESH	Crohn’s disease
disease	MESH	acute ischemic stroke

Original Article

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