Vol.:(0123456789)
Drugs
https://doi.org/10.1007/s40265-020-01443-4
REVIEW ARTICLE
Lefamulin: A Novel Oral and Intravenous Pleuromutilin
for the Treatment of Community‑Acquired Bacterial Pneumonia
George G. Zhanel
1
· Christina Deng
2
· Sheryl Zelenitsky
2
· Courtney K. Lawrence
2
· Heather J. Adam
1,3
·
Alyssa Golden
1
· Liam Berry
4
· Frank Schweizer
1,4
· Michael A. Zhanel
1
· Neal Irfan
5
· Denice Bay
1
·
Philippe Lagacé‑Wiens
1,3
· Andrew Walkty
1,3
· Lionel Mandell
6
· Joseph P. Lynch III
7
· James A. Karlowsky
1,3
© Springer Nature Switzerland AG 2020
Abstract
Lefamulin is a novel oral and intravenous (IV) pleuromutilin developed as a twice-daily treatment for community-acquired
bacterial pneumonia (CABP). It is a semi-synthetic pleuromutilin with a chemical structure that contains a tricyclic core of
five-, six-, and eight-membered rings and a 2-(4-amino-2-hydroxycyclohexyl)sulfanylacetate side chain extending from C14
of the tricyclic core. Lefamulin inhibits bacterial protein synthesis by binding to the 50S bacterial ribosomal subunit in the
peptidyl transferase center (PTC). The pleuromutilin tricyclic core binds to a pocket close to the A site, while the C14 side
chain extends to the P site causing a tightening of the rotational movement in the binding pocket referred to as an induced-
fit mechanism. Lefamulin displays broad-spectrum antibacterial activity against Gram-positive and Gram-negative aerobic
and anaerobic bacteria as well as against atypical bacteria that commonly cause CABP. Pleuromutilin antibiotics exhibit
low rates of resistance development and lack cross-resistance to other antimicrobial classes due to their unique mechanism
of action. However, pleuromutilin activity is affected by mutations in 23S rRNA, 50S ribosomal subunit proteins rplC and
rplD, ATP-binding cassette (ABC)-F transporter proteins such as vga(A), and the methyltransferase cfr. The pharmacokinetic
properties of lefamulin include: volume of distribution (V
d
) ranging from 82.9 to 202.8 L, total clearance (CL
T
) of 19.5 to
21.4 L/h, and terminal elimination half-life (t
1/2
) of 6.9–13.2 h; protein binding of lefamulin is high and non-linear. The
oral bioavailability of lefamulin has been estimated as 24% in fasted subjects and 19% in fed subjects. A single oral dose of
lefamulin 600 mg administered in fasted patients achieved a maximum plasma concentration (C
max
) of 1.2–1.5 mg/L with
a time of maximum concentration (T
max
) ranging from 0.8 to 1.8 h, and an area under the plasma concentration-time curve
from 0 to infinity (AUC
0−∞
) of 8.5–8.8 mg h/L. The pharmacodynamic parameter predictive of lefamulin efficacy is the free
plasma area under the concentration-time curve divided by the minimum inhibitory concentration (fAUC
24h
/MIC). Lefamu-
lin efficacy has been demonstrated using various animal models including neutropenic murine thigh infection, pneumonia,
lung infection, and bacteremia. Lefamulin clinical safety and efficacy was investigated through a Phase II clinical trial of
acute bacterial skin and skin structure infection (ABSSSI), as well as two Phase III clinical trials of CABP. The Phase III
trials, LEAP 1 and LEAP 2 established non-inferiority of lefamulin to moxifloxacin in both oral and IV formulations in the
treatment of CABP. The United States Food and Drug Administration (FDA), European Medicines Agency (EMA), and
Health Canada have each approved lefamulin for the treatment of CABP. A Phase II clinical trial has been completed for
the treatment of ABSSSI, while the pediatric program is in Phase I. The most common adverse effects of lefamulin include
mild-to-moderate gastrointestinal-related events such as nausea and diarrhea. Lefamulin represents a safe and effective option
for treating CABP in cases of antimicrobial resistance to first-line therapies, clinical failure, or intolerance/adverse effects to
currently used agents. Clinical experience and ongoing clinical investigation will allow clinicians and antimicrobial steward-
ship programs to optimally use lefamulin in the treatment of CABP.
Extended author information available on the last page of the article