Abstract P3-03-04: Establishment and characterization of ESR1-mutant breast cancer PDX models

Abstract: The estrogen receptor (ER or ESR1) drives proliferation and growth of luminal type breast cancers. Endocrine therapies are highly effective in a majority of these cancers types; however, disease progression eventually occurs due to acquired resistance resulting in hormone-independent breast cancer. One mechanism of resistance is acquired mutations at codons 537 and 538 in the ligand binding domain of the receptor which are found in ∼12% of pretreated, ER+ patients. These mutations result in constitutive ER act… Show more

“…44 Dual blockade of mTOR 1/2 and HER2 resulted in anti-tumor activity in in vitro pre-clinical models of breast cancer resistant to anti-HER2 therapies. 45 Garay et al 46 used the SK-BR3 cell line to demonstrate that only kinase domain (H1047R) mutations and not helical domain (E545K) mutations confer resistance to lapatinib. Le et al 47 investigated molecular mechanisms of resistance to PI3K inhibitors demonstrating that expression of proviral insertion site in murine leukaemia virus (PIM) is able to bypass AKT inhibition, thus conferring resistance to selective PI3Kα inhibitor BYL719/Alpelisib in BC cell lines.…”

The prognostic value of PI3K mutational status in breast cancer: A meta‐analysis

“…44 Dual blockade of mTOR 1/2 and HER2 resulted in anti-tumor activity in in vitro pre-clinical models of breast cancer resistant to anti-HER2 therapies. 45 Garay et al 46 used the SK-BR3 cell line to demonstrate that only kinase domain (H1047R) mutations and not helical domain (E545K) mutations confer resistance to lapatinib. Le et al 47 investigated molecular mechanisms of resistance to PI3K inhibitors demonstrating that expression of proviral insertion site in murine leukaemia virus (PIM) is able to bypass AKT inhibition, thus conferring resistance to selective PI3Kα inhibitor BYL719/Alpelisib in BC cell lines.…”

The prognostic value of PI3K mutational status in breast cancer: A meta‐analysis