Trilaciclib prior to chemotherapy reduces the usage of supportive care interventions for chemotherapy‐induced myelosuppression in patients with small cell lung cancer: Pooled analysis of three randomized phase 2 trials

Ferrarotto, Renata; Anderson, Ian C.; Medgyasszay, Balazs; Garcia-Campelo, M. Rosario; Edenfield, William J.; Feinstein, T. M.; Johnson, Jennifer M.; Kalmadi, Sujith; Lammers, Philip E.; Sánchez-Hernández, Alfredo; Pritchett, Yili; Morris, Shannon R.; Malik, Rajesh; Csőszi, Tibor

doi:10.1002/cam4.4089

Cited by 35 publications

(25 citation statements)

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“…Trilaciclib induces a transient, reversible G1 cell cycle arrest of proliferating hematopoietic stem and progenitor cells in bone marrow, thus protecting them from damage during chemotherapy. Its myeloprotection has been demonstrated in clinical studies for small cell lung cancer 20–22 . Trilaciclib effectively protects against neutropenia 21 and enhances the antitumor activity of chemotherapy and immune checkpoint inhibitor combinations 23 .…”

Section: Discussionmentioning

confidence: 99%

LP2, a stable lanthipeptide derived from cAng‐(1‐7), exerts myeloprotective action in mice

Namsolleck¹,

Rodgers

Franklin³

et al. 2023

European J of Haematology

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Objectives: Linear unstable angiotensins stimulate hematopoiesis. Here we address:(1) Is cyclic angiotensin-(1-7) myeloprotective in mice? (2) Is cyclic angiotensin-(1-7) stable in rat? (3) Does LP2, a cyclic angiotensin-(1-7) with an N-terminal D-lysine, exert myeloprotective action in tumor-bearing mice?Materials and Methods: Cyclic angiotensin-(1-7)'s capacity to restore levels of blood platelets and white blood cells was studied in gemcitabine-treated mice. The stability of cyclic angiotensin-(1-7) in rat was measured in blood samples taken after injection or infusion. The capacity of LP2 to restore total bone marrow cell levels in mice after treatment with 5-fluoruracil was measured. In addition, the capacity of LP2 to counter anemia in tumor-bearing mice treated with erlotinib was measured.Results: Cyclic angiotensin-(1-7) dose-dependently restored blood platelet levels in gemcitabine-treated mice, whereas its capacity to restore levels of white blood cells was less. In vivo aminoterminal breakdown of cyclic angiotensin-(1-7) yielded cyclic angiotensin-(2-7) and cyclic angiotensin-(3-7). LP2 significantly (p < .0001 at 100 μg/ kg/day) restored bone marrow cell counts in mice after treatment with 5-fluoruracil.LP2 also significantly (p < .05) countered anemia in tumor-bearing mice treated with erlotinib.Conclusions: LP2 exerts myeloprotective action with perspectives for continuation of its clinical development.

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Section: Discussionmentioning

confidence: 99%

LP2, a stable lanthipeptide derived from cAng‐(1‐7), exerts myeloprotective action in mice

Namsolleck¹,

Rodgers

Franklin³

et al. 2023

European J of Haematology

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“…Interestingly, in tumors predicted to be insensitive to CDK4/6i, transient administration of these drugs could be used to transiently arrest proliferation of normal cells and prevent chemotherapy-induced myelosuppression, hence allowing to increase the dose of genotoxic drugs such as cisplatin and thus the therapeutic window between normal and transformed cells (96). This idea has been validated clinically in small cell lung cancers that are generally insensitive to CDK4/6i due to their RB1 locus alteration (97), leading to recent approval by the FDA of trilaciclib for this indication. Therefore, defining or predicting the CDK4 phosphorylation status might really be one key to tailor the use of CDK4/6i in MPM treatment and their combination with targeted or genotoxic therapies.…”

Section: Discussionmentioning

confidence: 99%

Preclinical evaluation of CDK4 phosphorylation predicts high sensitivity of malignant pleural mesotheliomas to CDK4/6 inhibition

Paternot

Raspé

Meiller

et al. 2022

Preprint

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Malignant pleural mesothelioma (MPM) is an aggressive cancer with limited therapeutic options. In this study, we evaluated the impact of CDK4/6 inhibition by palbociclib in a panel of 28 MPM cell lines, including 19 patient-derived cell lines, using a variety of approaches including RNA-sequencing. Palbociclib used alone sufficed to strongly and durably inhibit the proliferation of 23 MPM cell lines, indicating a unique sensitivity of MPM to CDK4/6 inhibition. Importantly, insensitivity to palbociclib was mostly explained by the lack of active T172-phosphorylated CDK4. This was associated with the high p16INK4A (CDKN2A) levels that accompany RB1 defects or inactivation, and also (unexpectedly) cyclin E1 over-expression in the presence of wild-type RB1. Prolonged treatment with palbociclib irreversibly inhibited proliferation despite re-induction of cell cycle genes upon drug washout. A senescence-associated secretory phenotype including various potentially immunogenic components was also irreversibly induced. Phosphorylated CDK4 was detected in 80% of 47 MPM tumors indicating their intrinsic sensitivity to CDK4/6 inhibitors. The absence of this phosphorylation in some highly proliferative MPM tumors was linked to partial deletions of RB1, leading to very high p16 (CDKN2A) expression. Our study strongly supports the clinical evaluation of CDK4/6 inhibitory drugs for MPM treatment, in monotherapy or combination therapy.

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“…14,16,19,20 Administration of trilaciclib prior to chemotherapy also improved multiple other myelosuppression endpoints, including the incidence of grade 3/4 haematologic adverse events (AEs), and resulted in the need for fewer supportive care interventions, fewer dose modifications and improved quality of life. 14,16,[19][20][21] Antitumour efficacy outcomes were comparable in the trilaciclib and placebo arms, indicating that, while administration of trilaciclib prior to chemotherapy did not enhance antitumour efficacy in the setting of ES-SCLC, neither did it antagonize the intended effects of chemotherapy. 14,16,19 The recommended phase 2 dose (RP2D) and approved dose for trilaciclib in patients with ES-SCLC is 240 mg/m 2 , as established by analysis of integrated pharmacokinetic (PK), pharmacodynamic (PD),…”

Section: Introductionmentioning

confidence: 95%

“…In each individual trial and in a pooled analysis of all three trials, the addition of trilaciclib prior to standard chemotherapy significantly improved the primary endpoints of duration of severe neutropenia in cycle 1 and occurrence of severe neutropenia 14,16,19,20 . Administration of trilaciclib prior to chemotherapy also improved multiple other myelosuppression endpoints, including the incidence of grade 3/4 haematologic adverse events (AEs), and resulted in the need for fewer supportive care interventions, fewer dose modifications and improved quality of life 14,16,19–21 . Antitumour efficacy outcomes were comparable in the trilaciclib and placebo arms, indicating that, while administration of trilaciclib prior to chemotherapy did not enhance antitumour efficacy in the setting of ES‐SCLC, neither did it antagonize the intended effects of chemotherapy 14,16,19 …”

Section: Introductionmentioning

confidence: 99%

Population pharmacokinetics and exposure–response of trilaciclib in extensive‐stage small cell lung cancer and triple‐negative breast cancer

Rich

Bullock

et al. 2022

Brit J Clinical Pharma

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Aims: Trilaciclib is a first-in-class, intravenous cyclin-dependent kinase 4/6 inhibitor that provides multilineage protection from chemotherapy-induced myelosuppression. This analysis aimed to characterize the population pharmacokinetics (PK) of trilaciclib, identify potential covariates influencing trilaciclib PK, and evaluate exposureresponse relationships in extensive-stage small cell lung cancer (ES-SCLC) and triplenegative breast cancer (TNBC) trials.Methods: Population PK analysis was performed using data from healthy volunteers (n = 72), patients with ES-SCLC (n = 111) and patients with TNBC (n = 14).Exposure-response analyses were conducted to investigate the impact of trilaciclib exposure (AUC) on myeloprotective efficacy, antitumour efficacy and safety. Logistic regression and Cox regression models were used for binary and time-to-event endpoints, respectively.Results: Trilaciclib PK was described by a three-compartment model. Sex, body surface area, baseline albumin concentration and age were identified as significant covariates on trilaciclib PK but did not have clinically relevant impact on exposure. Based on exposure-response analyses, lower and higher exposures of trilaciclib at clinical doses (200-280 mg/m 2 ) were associated with similar myeloprotective effects. Trilaciclib exposure did not impact the antitumour effects of chemotherapy. Higher exposure to trilaciclib was associated with higher probabilities of headache, phlebitis/ thrombophlebitis and injection site reactions. Conclusion:No dose adjustments are required based on the covariates tested. Trilaciclib resulted in optimal myeloprotective effects with no impact on antitumour effects of chemotherapy. However, higher exposure increased the probabilities of adverse events. The data further support selection of the recommended phase 2 dose (trilaciclib 240 mg/m 2 ).

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Trilaciclib prior to chemotherapy reduces the usage of supportive care interventions for chemotherapy‐induced myelosuppression in patients with small cell lung cancer: Pooled analysis of three randomized phase 2 trials

Abstract: This is an open access article under the terms of the Creat ive Commo ns Attri bution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

Cited by 35 publications

References 32 publications

LP2, a stable lanthipeptide derived from cAng‐(1‐7), exerts myeloprotective action in mice

LP2, a stable lanthipeptide derived from cAng‐(1‐7), exerts myeloprotective action in mice

Preclinical evaluation of CDK4 phosphorylation predicts high sensitivity of malignant pleural mesotheliomas to CDK4/6 inhibition

Population pharmacokinetics and exposure–response of trilaciclib in extensive‐stage small cell lung cancer and triple‐negative breast cancer

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