摘要:Correction to:
Scientific Reports 10.1038/s41598-021-99184-1, published online 06 October 2021
The original version of this Article contained an error in Figure 3 and 4 where the graph for panel C was omitted. The original Figures
3 and
4 and accompanying legends appear below.
Figure 3
Synergism of ivacaftor (VX-770) and elexacaftor (VX-445) in potentiating G551D-CFTR in FRT cells. (
A) Representative I
t recordings of FRT cells expressing human G551D-CFTR showing acute actions of VX-770 and VX-445. (
B–C) Changes in I
t after acute addition of VX-770 in the absence and presence of VX-445 (
B) and in response to the acute addition of VX-445 in the absence and presence of VX-770 (
C). (
D–E) Changes in I
t after the additions of test compounds for the experiment presented in (
A). G551D-CFTR mediated I
t is greatest after acute potentiation by both VX-770 and VX-445. (
F) Representative I
t recordings of FRT cells expressing human G551D-CFTR treated for 24 h with DMSO, VX-770, and/or VX-445. (
G) Changes in I
t after the additions of test compounds for the experiment presented in (
F). G551D-CFTR mediated I
t is greatest after chronic treatment by both VX-770 and VX-445. See SI for additional experimental details and for supporting data. All data are presented as mean ± standard error. Bars with different letters (A, B, C…) are significantly different from each other (ANOVA;
P < 0.05). Asterisks indicate specific
P values: ****
P < 0.0001.
Figure 4
Synergism of ivacaftor (VX-770) and elexacaftor (VX-445) in potentiating G551D-CFTR in HNE cells. (
A) Representative I
t recordings of G551D-HNE cells showing acute actions of VX-770 and VX-445. (
B–C) Changes in I
t after acute addition of VX-770 in the absence and presence of VX-445 (
B) and in response to the acute addition of VX-445 in the absence and presence of VX-770 (
C). (
D–E) Changes in I
t after the additions of test compounds for the experiment presented in (
A). G551D-CFTR mediated I
t is greatest after acute potentiation by both VX-770 and VX-445. (
F) Representative I
t recordings of G551D-HNE treated for 24 h with DMSO, the double combination of VX-770 and VX-445, or the triple combination of VX-661, VX-770, and VX-445 (i.e., Trikafta). (
G) CFTR
inh-172 inhibited I
t for the experiment presented in (
F). See SI for additional experimental details and for supporting data. All data are presented as mean ± standard error. Bars with different letters (A, B, C…) are significantly different from each other (ANOVA;
P < 0.05). Asterisks indicate specific
P values: ****
P < 0.0001.
The original Article has been corrected.
