Incidence of Cutaneous Adverse Events With Phosphoinositide 3-Kinase Inhibitors as Adjuvant Therapy in Patients With Cancer

Abstract: ImportanceThe phosphoinositide 3-kinase (PI3K) pathway is among the most frequently activated pathways in human cancers. As the use of PI3K inhibitors for cancer treatment grows, there is increasing need for understanding the cutaneous effects associated with these therapies.ObjectiveTo systematically review the published literature reporting incidence of cutaneous adverse events with PI3K inhibitors and to provide pooled incidence estimates using meta-analysis.Data SourcesThis systematic review and meta-analy… Show more

“…In addition, we originally reported that subgroup analyses found an inconclusively higher incidence of severe rashes with the use of Pan-class compared with isoform-selective PI3K inhibitors; corrected subgroup analyses revealed that the incidence of severe rashes did not differ significantly between classes of PI3K inhibitors. These corrections do not change the overall results and conclusions of our study, 1 which continues to find an increased risk of all-grade and severe-grade (3-5) eruptions associated with PI3K inhibitors.…”

“…We defined rashes according to the Common Terminology Criteria for Adverse Events (CTCAE v 5.0). We appreciate Wu and colleagues' attention to detail and have added severe-grade rash data from the studies by Zelenetz et al study, Vuylsteke et al, and Bowles et al 1 In addition, we have corrected data for severe grade rash reported in the study by Powles et al 1 These corrections to the data on severe grade rash resulted in an increase to 17 trials comprising 4429 participants vs the originally reported 14 trials and 3750 participants; a change to no evidence of statistical heterogeneity (I 2 = 0%, Q = 7.16) from our previously reported significant statistical heterogeneity (I 2 = 43.62%, Q = 23.06); and a change in the pooled Peto odds ratio (OR) to 6.36 (95% CI, 4.58-8.83) and incidence of 3.41% from the originally reported pooled Peto OR of 4.64 (95% CI, 2.70-7.97) and incidence of 6.95%. In addition, we originally reported that subgroup analyses found an inconclusively higher incidence of severe rashes with the use of Pan-class compared with isoform-selective PI3K inhibitors; corrected subgroup analyses revealed that the incidence of severe rashes did not differ significantly between classes of PI3K inhibitors.…”

“…For our review, 1 we dichotomized results for the frequency of rashes into 2 groups according to their severityeither any grade or severe grade (3)(4)(5). We defined rashes according to the Common Terminology Criteria for Adverse Events (CTCAE v 5.0).…”

“…Exceptions have been made, using continuity corrections. With reference to the studies by Levy et al and Jimeno et al, 1 we included these studies with zero events in our severe rash analyses because a continuity correction of 0.5 was applied in both of those studies. This was specifically referenced in our study's Methods section.…”

“…This was specifically referenced in our study's Methods section. The forest plot mentioned zero frequency as 1 for Levy et al, 1 and for the study by Jimeno et al the software rounded off 0.5 (continuity correction) to 1. This is also intuitive because a frequency of 0.5 would not make sense to the readers.…”

Validity of Meta-Analytical Data on Cutaneous Adverse Events with Phosphoinositide 3-Kinase Inhibitors—Reply

“…In addition, we originally reported that subgroup analyses found an inconclusively higher incidence of severe rashes with the use of Pan-class compared with isoform-selective PI3K inhibitors; corrected subgroup analyses revealed that the incidence of severe rashes did not differ significantly between classes of PI3K inhibitors. These corrections do not change the overall results and conclusions of our study, 1 which continues to find an increased risk of all-grade and severe-grade (3-5) eruptions associated with PI3K inhibitors.…”

“…We defined rashes according to the Common Terminology Criteria for Adverse Events (CTCAE v 5.0). We appreciate Wu and colleagues' attention to detail and have added severe-grade rash data from the studies by Zelenetz et al study, Vuylsteke et al, and Bowles et al 1 In addition, we have corrected data for severe grade rash reported in the study by Powles et al 1 These corrections to the data on severe grade rash resulted in an increase to 17 trials comprising 4429 participants vs the originally reported 14 trials and 3750 participants; a change to no evidence of statistical heterogeneity (I 2 = 0%, Q = 7.16) from our previously reported significant statistical heterogeneity (I 2 = 43.62%, Q = 23.06); and a change in the pooled Peto odds ratio (OR) to 6.36 (95% CI, 4.58-8.83) and incidence of 3.41% from the originally reported pooled Peto OR of 4.64 (95% CI, 2.70-7.97) and incidence of 6.95%. In addition, we originally reported that subgroup analyses found an inconclusively higher incidence of severe rashes with the use of Pan-class compared with isoform-selective PI3K inhibitors; corrected subgroup analyses revealed that the incidence of severe rashes did not differ significantly between classes of PI3K inhibitors.…”

“…For our review, 1 we dichotomized results for the frequency of rashes into 2 groups according to their severityeither any grade or severe grade (3)(4)(5). We defined rashes according to the Common Terminology Criteria for Adverse Events (CTCAE v 5.0).…”

“…Exceptions have been made, using continuity corrections. With reference to the studies by Levy et al and Jimeno et al, 1 we included these studies with zero events in our severe rash analyses because a continuity correction of 0.5 was applied in both of those studies. This was specifically referenced in our study's Methods section.…”

“…This was specifically referenced in our study's Methods section. The forest plot mentioned zero frequency as 1 for Levy et al, 1 and for the study by Jimeno et al the software rounded off 0.5 (continuity correction) to 1. This is also intuitive because a frequency of 0.5 would not make sense to the readers.…”

Validity of Meta-Analytical Data on Cutaneous Adverse Events with Phosphoinositide 3-Kinase Inhibitors—Reply

Use of Artificial Intelligence Chatbots for Cancer Treatment Information

Validity of Meta-Analytical Data on Cutaneous Adverse Events With Phosphoinositide 3-Kinase Inhibitors