PI3K INHIBITORS

Pan-PI3K Inhibitors

Early strategies of inhibiting PI3K have involved pan-inhibition of all four PI3K isoforms. Pan-inhibition can potentially be effective in a broad range of tumor types, but it can also be associated with greater toxicity.

Buparlisib

Buparlisib is an oral pan PI3K inhibitor.¹⁴ The BELLE-2 study was a randomized, double-blind- placebo controlled Phase 3 study evaluating the efficacy of buparlisib in breast cancer.¹⁴ In this study, 1147 patients with HR+/HER2 negative inoperable locally advanced or MBC whose disease had progressed on or after AI and who had received up to one previous line of chemotherapy were included. Patients were randomly assigned to receive fulvestrant with or without buparlisib. The addition of buparlisib improved median PFS in the total patient population from 5.0 months to 6.9 months (HR 0.78, p=0.00021). In patients with PI3K activated pathway, median PFS was 6.8 months in the combination group compared with 4.0 months in fulvestrant alone group (HR 0.76, p=0.014). The most common grade 3–4 adverse events (AEs) in the combination group were increased liver functions tests (LFTs), hyperglycemia and rash.¹⁴

In the phase III BELLE-3 study, 432 post-menopausal women were randomly assigned to fulvestrant with or without the addition of buparlisib. Patients had HR+/HER2 negative locally advanced or MBC who had relapsed on or after endocrine therapy and mTOR inhibitor. The addition of buparlisib led to improvement in median PFS from 1.8 months to 3.9 months (HR 0.67, p=0.00030). The most frequent grade 3–4 AEs in the buparlisib group included elevation in LFTs, hypertension and fatigue.¹⁵ Due to toxicities and safety issues with only modest PFS improvement, this drug did not move forward in further development.

Pictilisib

Pictilisib is also a pan PI3K inhibitor. The phase II PEGGY trial randomized 183 pre- and post-menopausal patients with HR+/HER2 negative MBC to receive chemotherapy (paclitaxel) with either pictilisib or placebo. There was no statistically significant improvement in PFS with the addition of pictilisib. In the intention to treat (ITT) population, median PFS was 7.8 months in the placebo group compared with 8.2 months with the addition of pictilisib (HR 0.95, p = 0.83). In patients with PIK3CA mutation, the median PFS was 5.8 months in the placebo group compared with 7.3 months with the addition of pictilisib (HR 1.06, p = 0.88). Pictilisb was associated with more frequent serious AEs and dose reductions/discontinuations compared to placebo.¹⁶

Isoform-Specific PI3K Inhibitors

Isoform-specific PI3K inhibitors may offer the opportunity for higher doses and potentially greater efficacy with less toxicity compared to pan PI3K inhibitor.¹¹ Taselisib is a beta-sparing PI3K inhibitor that was studied in the phase III SANDPIPER clinical trial.¹⁷ In this study, 516 postmenopausal women were randomized to fulvestrant plus placebo or fulvestrant plus taselisib. The combination treatment group improved investigator assessed PFS from 5.4 months to 7.4 months (HR 0.70, p = 0.0037). The most common grade 3/4 AEs included diarrhea, hyperglycemia, colitis and stomatitis.¹⁷

Alpelisib in the Treatment of PIK3CA Mutated Breast Cancer

Following preclinical data demonstrating tolerability and efficacy of alpelisib, the first in human phase Ia study was performed to show efficacy and tolerability of alpelisib in PIK3CA altered advanced solid tumors.¹⁸ In this study, 134 patients with unresectable, advanced solid tumors were enrolled. The most common solid tumor types were breast (26.9%), colorectal (26.1%) and head and neck (14.2%). Results showed favorable safety profile up to 400mg daily dose and 150mg twice daily dose. Objective tumor response was observed at a dose of 270mg or higher once daily. Overall response rate was seen in 8 patients (6.0%), with partial response seen in seven patients and one complete response. In patients with HR+/HER2 negative breast cancer, median PFS was 5.5 months. The most commons AEs included hyperglycemia (52%), nausea (51%), decreased appetite (42%), diarrhea (40%) and vomiting (31%). In the dose escalation phase, dose limiting toxicities (DLTs) occurred in nine total patients. DLTs included hyperglycemia (n=2 at 450mg once daily dose and n=4 at 200mg twice daily dose), nausea (n=2 at 450mg once daily dose) and combined hyperglycemia and hypophosphatemia (n=1 at 150mg twice daily dose).¹⁸

As stated previously, the incidence of PIK3CA mutation in HR+ breast cancer is approximately 35%.^11,13 PI3K inhibition by alpelisib has been shown to cause an increase in estrogen receptor transcription in breast cancer cells.¹⁹ Therefore, one strategy that has been studied is combination of PI3K inhibitor with endocrine therapy in PIK3CA mutated HR+ breast cancers in order to achieve greater sustained therapeutic response compared to endocrine therapy alone.²⁰ In a phase Ib study, escalating once-daily doses of alpelisib (300mg, 350mg and 400mg) in combination with fixed dose fulvestrant (500 mg) was studied in 87 postmenopausal women with PIK3CA altered or PIK3CA wild type HR positive MBC.²⁰ Patients had received a median of five prior lines of antineoplastic therapy. The maximum tolerated dose (MTD) was 400mg and the 300mg once daily dose was determined to be the recommended Phase 2 dose. The median PFS in PIK3CA altered group with alpelisib was 9.1 months (95% CI, 6.6–14.6) versus 4.7 months (95% CI, 1.9–5.6) in wild type group. Overall response rate in the PIK3CA altered group was 29% and no objective tumor response was observed in the wild type group. The most common grade 3–4 AEs with alpelisib 400mg once daily dosing included hyperglycemia (22%) and maculopapular rash (13%).²⁰

With evidence of the efficacy and tolerability of alpelisib as monotherapy and in combination with endocrine therapy, a phase 3 study was performed to further confirm these findings.²¹ The SOLAR −1 study was a randomized phase 3 study that sought to evaluate the efficacy and safe of alpelisib plus fulvestrant in patients with PIK3CA mutated HR+/HER2 negative who had received prior endocrine therapy but no prior chemotherapy.²¹ A total of 572 patients were enrolled in the study, 341 patients had a PIK3CA mutation. At a median follow-up of 20 months, the median PFS in patients with PIK3CA mutation was 11.0 months in the alpelisib plus fulvestrant combination group compared with 5.7 months in the fulvestrant alone group (HR 0.65, p<0.001). Overall response rate in patients with PIK3CA mutation was 26.6% in the combination group compared to 12.8% in the fulvestrant alone group. The most frequent grade 3–4 AEs in the alpelisib plus fulvestrant cohort included hyperglycemia (36.6%) and rash (9.9%). Grade 3 diarrhea occurred in 6.7% of patients in the combination group. No grade 4 diarrhea was reported. The rate of discontinuation in the combination group was 25% compared to 4.2% in fulvestrant alone group.²¹ The results from the SOLAR-1 phase 3 study led to the FDA approval on May 24, 2019 of alpelisib in combination with fulvestrant for postmenopausal women and men with HR+/HER2 negative, PIK3CA-mutated advanced or metastatic breast cancer following progression on or after an endocrine-based regimen.¹⁹

Mechanisms of Resistance and Mechanisms of Enhanced Response to Alpelisib

There are multiples mechanisms of resistance to PI3K inhibitors. The effect of isoform specific PI3K inhibitors, like alpelisib, can be circumvented by activating other isoforms and thereby promoting downstream signaling of the PI3K/AKT/mTOR pathway.²² Additional mechanisms include activation of downstream effectors like AKT or mTOR.²²

Loss of PTEN has also been shown to be a cause of resistance to PI3K inhibitors. In one study, circulating tumor DNA (ctDNA) and tumor tissue was analyzed from patients with HR+/HER2 negative MBC who participated in a phase I/II trial of alepelisib in combination with AI.²³ The authors sought to identify mechanisms of resistance that could explain why a subset of patients lacked clinical benefit to alpelisib and rapidly progressed following initiation of treatment. Clinical benefit was only observed in patients who harbored a PIK3CA mutation. CtDNA was then used to identify PTEN mutations in 25% of patients. Three of these patients had PTEN loss in pre-treatment samples and all of whom had rapid progression of disease after start of treatment with alpelisib and AI therapy. It was also discovered in tumor xenograft models that mutations in ESR1 led to rapid progression following start of alpelisib and AI therapy. Further supporting the idea that there is cross talk between PI3K and ER signaling and mutations in ESR1 can further promote resistant and contribute to progression of disease.²³

While there are mechanisms of resistance to alpelisib, there are also mechanisms of enhanced response to this therapy. 10–15% of all PIK3CA mutant tumors across all cancer types contain multiple PIK3CA mutations, mainly double PIK3CA mutations.²⁴ Double PIK3CA mutations are commonly found in HR+/HER2 negative breast cancers. Double mutations in cis have shown to increase downstream PI3K pathway signaling and cell/tumor proliferation compared to single mutations. An analysis was performed looking at the ctDNA from the SANDPIPER study to detect the presence of PIK3CA mutations. Patients with a single PIK3CA mutation receiving taselisib had an overall response rate of 18.1%. But patients with multiple PIK3CA mutations receiving taselisib had overal response rate of 30.2%.²⁴

Taken together, the above data suggest that identification of other mutations (ie, ESR1, PTEN) in addition to PIK3CA and quantifying the number of unique PIK3CA mutations may be necessary in order to create tailored therapeutic strategies for patients with HR+/HER2 negative MBC.

PIK3CA Mutation Testing

The FDA has approved the Therascreen^® PIK3CA mutation assay for detection of PIK3CA mutation in patients.²⁵ This diagnostic test was used in the SOLAR-1 study and it detects 11 PIK3CA mutations in tumor tissue specimens and/or in ctDNA.²¹ However, there is considerable heterogeneity of PIK3CA mutations in breast cancer and there could potentially be additional PIK3CA mutations that have important clinical implications and are not detected on the Therascreen^® assay. In one study, the Therascreen^® panel detected four common PIK3CA mutations (H1047R, E545K, E542K, H1047L) comprising 67% of all PIK3CA mutations in the study dataset.²⁵ Furthermore, the Therascreen^® assay was shown to detect 80% of patients who have a known PIK3CA mutation. In patients known to harbor double PIK3CA mutation, the Therascreen^® assay identified both PIK3CA mutations in only 5% of patients.²⁵ This study points to limitations of the Therascreen^® assay and potentially 20% of patients with a known PIK3CA mutation would go undetected. Furthermore, it is unclear the clinical importance and benefit of alpelisib therapy in patients with PIK3CA mutations that are not identified by the Therascreen^® assay but may be detected on other next-generation sequencing assays.

Administration/Safety and Toxicity

The starting dose of alpelisib is 300mg once daily. There are two dose reductions available which are 250mg once daily and 200mg once daily. Fulvestrant is administered 500mg IM on days 1, 15 and 29 and one monthly thereafter.¹⁹

The most frequent grade 3–4 AEs observed in patients who received alpelisib included hyperglycemia, severe cutaneous reaction and diarrhea. Additional adverse reactions that are listed in the FDA prescribing information include severe hypersensitivity and pneumonitis. Specific monitoring guidelines have been established to address these side effects. All patients must have a fasting plasma glucose (FPG) and HbA1C prior to initiation with alpelisib. FPG is then monitored once every week for the first 2 week and then at least every 4 weeks. HbA1c is monitored every 3 months and as clinically indicated. Patients with a history of controlled type 2 diabetes were included in SOLAR-1 trial but patients with type 1 and uncontrolled type 2 diabetes were excluded. Patients who develop grade 1 or greater hyperglycemia are recommended to initiate or intensify anti-hyperglycemia treatment.¹⁹

Severe cutaneous reaction including Stevens-Johnson syndrome (SJS) and erythema multiforme (EM) were reported in 0.4% and 1.1% of patients in SOLAR-1 study, respectively. Specific guidelines are outlined for patients who may develop cutaneous reaction, including initiation of topical and/or oral corticosteroids and oral antihistamines and interruption or permanent discontinuation of alpelisib. In a subgroup of patients in the SOLAR-1 study, 86 patients received prophylaxis including antihistamines and the incidence of all grade rash was 27% versus 54% in the overall population. Similarly, the incidence of grade 3 rash was 12% in the group of patients receiving prophylactic antihistamine compared to 20% in overall population. Therefore, prophylactic antihistamine is a consideration in patients initiating alpelisib.¹⁹

Diarrhea of all grades occurred in 58% of patients in the SOLAR-1 study and 6.7% patients experienced grade 3 diarrhea. There were no episodes of grade 4 diarrhea. Recommendations for the management of diarrhea include initiating and/or intensifying antidiarrheal medications and interruption alpelisib therapy.¹⁹

Pneumonitis is a less common adverse event with it occurring in 1.8% of patients receiving alpelisib in SOLAR-1 study. Symptoms such as shortness of breath, cough, or interstitial infiltrates on radiologic exam raise concern for pneumonitis in patients on alpelisib. Permanent discontinuation of alpelisib is advised in any patient who develops pneumonitis.¹⁹

READ FULL ARTICLE From DovePress

Alpelisib in the Treatment of Breast Cancer: A Short Review on the Emerging Clinical Data