Plasma thymidine kinase 1 activity and outcome of ER+ HER2− metastatic breast cancer patients treated with palbociclib and endocrine therapy

Endocrine therapy is the cornerstone of treatment of estrogen receptor-positive (ER+) HER2-negative (HER2−) breast cancer [1]. Endocrine therapies for metastatic breast cancer (MBC) have remained largely unchanged for the past two decades. They include tamoxifen, aromatase inhibitors (AI), and fulvestrant. More recently, CDK4/6 inhibitors (palbociclib, ribociclib, abemaciclib) have been shown to be effective in ER+ HER2− MBC as first-line therapy in combination with letrozole [2‐4] or fulvestrant (a selective ER degrader) after progression on AI [5, 6]. However, no biomarker is currently validated to guide the use of these new drugs in clinical practice.

Thymidine kinase 1 (TK1) plays a crucial role in DNA synthesis and cell proliferation [7, 8]. In preliminary studies using the same assay, serum or plasma TK1 activity (sTKa, pTKa) was reported to be a prognostic circulating biomarker in early and advanced breast cancer [9‐12]. The prognostic impact of baseline serum TK1 levels and TK1 variation in response to therapy was also reported in 159 samples from a phase III trial comparing AI and fulvestrant in ER+ HER2− MBC [13].

We report here the prognostic impact of pTKa, assessed in a prospective study on ER+ HER2− MBC patients treated with endocrine therapy and CDK4/6 inhibitor.

To our knowledge, this is the largest study in ER+ HER2− MBC demonstrating the prognostic impact of pTKa at baseline and at 4 weeks in patients treated with endocrine therapy plus CDK4/6 inhibitors.

TK1 is an enzyme that is active during the cell cycle, especially during DNA synthesis. Its primary role is to catalyze thymidine into thymidine monophosphate. A low level of TKa is observed in resting cells, but TKa starts to increase during G1/S phase to reach its highest level during S phase and then disappears at mitosis. Several studies have shown that TKa is higher in cancer patients than in the healthy population [15], including in patients with breast cancer [14, 16].

Previous studies in BC have demonstrated a correlation between KI67 and serum TKa [17]. In ER+ HER2− BC treated with anastrozole and palbociclib in the neoadjuvant setting, Bagegni et al. showed that the sensitivity and specificity of the decrease in serum TKa to predict tumor Ki-67 reduction in response to palbociclib were 94.1% (95%CI [86.2–100%]) and 84% (95%CI [69.6–98.4%]), respectively. As Ki67 is known to be a biomarker of tumor response at 15 days from initiation of ET but requires a tumor biopsy, determination of pTKa could be a non-invasive way of measuring this response. In the present study, we did not observe any association between TKa and tumor Ki67 or SBR grade, which could be explained by the time-lag between determination of Ki67 or SBR grade, assessed on the primary tumor, and determination of pTKa in an advanced metastatic setting (as no tumor biopsy of metastasis was available at the start of ET+ CDK4/6 treatment).

Plasma or serum TKa has been shown to be a prognostic factor in other metastatic cancers [18‐20]. Several studies have been conducted in various MBC settings using the same assay (DiviTum) [21]. In 198 MBC patients (mostly HER2-negative) treated with chemotherapy, Bjöhle et al. showed that pretreatment serum TKa predicted PFS and OS in multivariate analysis (OS, HR = 1.81, 95%CI [1.26–2.61], p = 0.001, with a cutoff of 235 Du/L) [22]. Larsson et al. also demonstrated a significant association between pTKa and PFS and OS in univariate and multivariate analyses at baseline and at 1, 3, and 6 months in women with MBC receiving first-line systemic therapy [23]. In ER+ HER2− MBC treated with ET only, sTKa was shown to be a prognostic factor at baseline and during treatment in the EFECT trial [13], in which the median time to progression for patients (N = 111) with low baseline serum TKa levels (<  97 Du/L) was 5.03 months (95% confidence interval [CI] 3.9–5.9) versus 2.57 months (95%CI 2.0–3.5) in patients with high baseline serum TKa levels (p < 0.0001). A smaller cohort of 31 patients, mostly previously untreated for MBC, also showed a prognostic value of pTKa for PFS with a cutoff of 122 Du/L [24]. We have confirmed the prognostic impact of pTKa on PFS and OS in MBC ER+ HER2− patients treated with ET + CDK4/6, both at baseline and at 4 weeks, even if baseline pTKa remained the most powerful prognostic factor at 4 weeks. Thus, the 4-week value seems to have less interest when the baseline has been obtained.

The EFECT trial [13] suggested that patients whose sTKa increased from baseline while on endocrine therapy had a significantly shorter time to progression (3.39 months, 95%CI 2.14–4.11) than those in whom sTKa did not increase (5.39 months, 95%CI 4.01–6.68) (p = 0.0045). More recently, the TREnd trial [25] showed a significant correlation between the 4-week variation of pTKa and PFS in ER+/HER2− MBC patients treated with palbociclib (alone or in combination with endocrine therapy following progression during a previous line of therapy). In the TREnd study, pTKa increase (n = 33 patients) was associated with shorter PFS (median PFS for the group with increasing pTKa = 3.0 months, 95%CI [2.7-NA] versus 9 months for stable or decreasing pTKa, 95%CI [5.8–12.0], p = 0.002). Bonechi et al. also showed that patients with decreasing pTKa activity after 1 month of treatment had a significantly better PFS comparatively to the increasing pTKa group (14.5 months versus 3.8 months, respectively, p = 0.0026) [24]. In contrast, no significant association was observed between baseline pTKa and PFS. In the present study, we did not find a predictive impact of the variation of pTKa between baseline and 4 weeks, regardless of the increase/decrease cutoff used (data not shown), unlike these other studies [13, 24, 25]. These contradictory results could be explained by several factors. First, the patient population, particularly with regard to the number of lines of chemotherapy received at the time of inclusion. In our study, 20% of patients received at least 3 lines of chemotherapy and 33% received 1 or 2 lines. In constrast the patients included in the TREnd trial had received a maximum of only one line (18%) and those in Bonechi’s study were mostly chemotherapy-naive (67.7%) or had a maximum of 2 lines. Thus, patients in our study appeared to be at a more advanced stage of disease, with tumors becoming resistant to multiple lines of treatment, leading to increased cell proliferation. This might explain a higher median pTKa at baseline compared to the other studies (292 Du/L vs 75–122 Du/L in other studies), although the rate of visceral metastases was globally similar. Because of these differences in median pTKa across studies and clinical settings, a pTKa threshold should be defined according to treatment history and using a large and homogeneous population, for a better assessment of the prognostic impact of baseline pTKa and pTKa variation. Importantly, chemotherapy having been reported to increase TKa levels [26, 27], the early interpretation of the variation could be challenging and this might explain that the variation of pTKa level was not a prognostic factor here. Ongoing large studies like SWOG S0226 (NCT00075764), resistance to first-line therapy with an AI and palbociclib at Johns Hopkins (NCT03439735), and the PYTHIA study (NCT02536742) will address this. Another difference between our study and previous studies was the number of patients included in these studies, which was lower in Bonechi’s study (N = 29) and TREnd (N = 41) than in our study (N = 85). Concerning the timepoint, in the EFECT trial, the second time point was collected at 3 months and not at 4 weeks, which could also explain a discrepancy with this study.

The limitations of this study include the lack of power and the heterogeneity of patients, especially in terms of the number of previous lines of ET+ CDK4/6 inhibitor therapy, making it difficult to compare pTKa cutoffs to predict outcome between the various studies. The results of prospective studies with a homogeneous cohort, receiving first-line or second-line CDK4/6 inhibitors are eagerly awaited (NCT03439735 and NCT02536742), as well as an interventional study to define patients in which ET+ CDK4/6 inhibitors should be intensified or could be de-escalated in the case of poor tolerability while maintaining a good prognosis.

This study demonstrates the clinical validity of pTKa as a new circulating prognostic marker for PFS and OS in ER+ HER2− MBC patients treated with endocrine therapy and palbociclib. The clinical utility of this promising biomarker needs to be determined in an adequately designed prospective trial of combined targeted and endocrine therapies.