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Spotlight on isavuconazole in the treatment of invasive aspergillosis and mucormycosis: design, development, and place in therapy.
Abstract
In recent decades, important advances have been made in the diagnosis and treatment
of invasive aspergillosis (IA) and mucormycosis. One of these advances has been the
introduction of isavuconazole, a second-generation broad spectrum triazole with a
favorable pharmacokinetic and safety profile and few drug-drug interactions. Phase
III trials in patients with IA and mucormycosis demonstrated that isavuconazole has
similar efficacy to voriconazole for the treatment of IA (SECURE trial) and liposomal
amphotericin B for the treatment of mucormycosis (VITAL trial with subsequent case-control
analysis) and a favorable safety profile with significantly fewer ocular, hepatobiliary,
and skin and soft tissue adverse events compared to voriconazole. As a result, recent
IA guidelines recommend isavuconazole (together with voriconazole) as gold standard
treatment for IA in patients with underlying hematological malignancies. In contrast
to liposomal amphotericin B, isavuconazole can be safely administered in patients
with reduced renal function and is frequently used for the treatment of mucormycosis
in patients with reduced renal function. Updated guidelines on mucormycosis are needed
to reflect the current evidence and give guidance on the use of isavuconazole for
mucormycosis. Studies are needed to evaluate the role of isavuconazole for 1) anti-mold
prophylaxis in high-risk patients, 2) salvage treatment for IA and mucormycosis, and
3) treatment for other mold infections such as Scedosporium apiospermum.
Type
Journal articlePermalink
https://hdl.handle.net/10161/28630Published Version (Please cite this version)
10.2147/dddt.s145545Publication Info
Jenks, Jeffrey D; Salzer, Helmut Jf; Prattes, Juergen; Krause, Robert; Buchheidt,
Dieter; & Hoenigl, Martin (2018). Spotlight on isavuconazole in the treatment of invasive aspergillosis and mucormycosis:
design, development, and place in therapy. Drug design, development and therapy, 12. pp. 1033-1044. 10.2147/dddt.s145545. Retrieved from https://hdl.handle.net/10161/28630.This is constructed from limited available data and may be imprecise. To cite this
article, please review & use the official citation provided by the journal.
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Jeffrey Daniel Jenks
Adjunct Associate Professor in the Department of Medicine

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