Selective RET kinase inhibition for patients with RET-altered cancers

V. Subbiah; V. Velcheti; B. B. Tuch; K. Ebata; N. L. Busaidy; M. E. Cabanillas; L. J. Wirth; S. Stock; S. Smith; V. Lauriault; S. Corsi-Travali; D. Henry; M. Burkard; R. Hamor; K. Bouhana; S. Winski; R. D. Wallace; D. Hartley; S. Rhodes; M. Reddy; B. J. Brandhuber; S. Andrews; S. M. Rothenberg; A. Drilon

doi:10.1093/annonc/mdy137

Selective RET kinase inhibition for patients with RET-altered cancers

V. Subbiah, V. Velcheti, B. B. Tuch, K. Ebata, N. L. Busaidy, M. E. Cabanillas, L. J. Wirth, S. Stock, S. Smith, V. Lauriault, S. Corsi-Travali, D. Henry, M. Burkard, R. Hamor, K. Bouhana, S. Winski, R. D. Wallace, D. Hartley, S. Rhodes, M. ReddyB. J. Brandhuber, S. Andrews, S. M. Rothenberg, A. Drilon

Research output: Contribution to journal › Article › peer-review

292 Scopus citations

Abstract

Background: Alterations involving the RET kinase are implicated in the pathogenesis of lung, thyroid and other cancers. However, the clinical activity of multikinase inhibitors (MKIs) with anti-RET activity in RET-altered patients appears limited, calling into question the therapeutic potential of targeting RET. LOXO-292 is a selective RET inhibitor designed to inhibit diverse RET fusions, activating mutations and acquired resistance mutations. Patients and methods: Potent anti-RET activity, high selectivity, and central nervous system coverage were confirmed preclinically using a variety of in vitro and in vivo RET-dependent tumor models. Due to clinical urgency, two patients with RETaltered, MKI-resistant cancers were treated with LOXO-292, utilizing rapid dose-titration guided by real-time pharmacokinetic assessments to achieve meaningful clinical exposures safely and rapidly. Results: LOXO-292 demonstrated potent and selective anti-RET activity preclinically against human cancer cell lines harboring endogenous RET gene alterations; cells engineered to express a KIF5B-RET fusion protein -/+ the RET V804M gatekeeper resistance mutation or the common RET activating mutation M918T; and RET-altered human cancer cell line and patient-derived xenografts, including a patient-derived RET fusion-positive xenograft injected orthotopically into the brain. A patient with RET M918T-mutant medullary thyroid cancer metastatic to the liver and an acquired RET V804M gatekeeper resistance mutation, previously treated with six MKI regimens, experienced rapid reductions in tumor calcitonin, CEA and cell-free DNA, resolution of painful hepatomegaly and tumor-related diarrhea and a confirmed tumor response. A second patient with KIF5B-RET fusionpositive lung cancer, acquired resistance to alectinib and symptomatic brain metastases experienced a dramatic response in the brain, and her symptoms resolved. Conclusions: These results provide proof-of-concept of the clinical actionability of RET alterations, and identify selective RET inhibition by LOXO-292 as a promising treatment in heavily pretreated, multikinase inhibitor-experienced patients with diverse RET-altered tumors.

Original language	English (US)
Pages (from-to)	1869-1876
Number of pages	8
Journal	Annals of Oncology
Volume	29
Issue number	8
DOIs	https://doi.org/10.1093/annonc/mdy137
State	Published - Aug 2018

Keywords

RET
TKI
gatekeeper
multiknase inhibitor
targeted kinase inhibitor

ASJC Scopus subject areas

Hematology
Oncology

Access to Document

10.1093/annonc/mdy137

Cite this

Subbiah, V., Velcheti, V., Tuch, B. B., Ebata, K., Busaidy, N. L., Cabanillas, M. E., Wirth, L. J., Stock, S., Smith, S., Lauriault, V., Corsi-Travali, S., Henry, D., Burkard, M., Hamor, R., Bouhana, K., Winski, S., Wallace, R. D., Hartley, D., Rhodes, S., ... Drilon, A. (2018). Selective RET kinase inhibition for patients with RET-altered cancers. Annals of Oncology, 29(8), 1869-1876. https://doi.org/10.1093/annonc/mdy137

Subbiah, V, Velcheti, V, Tuch, BB, Ebata, K, Busaidy, NL , Cabanillas, ME, Wirth, LJ, Stock, S, Smith, S, Lauriault, V, Corsi-Travali, S, Henry, D, Burkard, M, Hamor, R, Bouhana, K, Winski, S, Wallace, RD, Hartley, D, Rhodes, S, Reddy, M, Brandhuber, BJ, Andrews, S, Rothenberg, SM & Drilon, A 2018, 'Selective RET kinase inhibition for patients with RET-altered cancers', Annals of Oncology, vol. 29, no. 8, pp. 1869-1876. https://doi.org/10.1093/annonc/mdy137

@article{00bfe84cdac045168761bf34906bb457,

title = "Selective RET kinase inhibition for patients with RET-altered cancers",

abstract = "Background: Alterations involving the RET kinase are implicated in the pathogenesis of lung, thyroid and other cancers. However, the clinical activity of multikinase inhibitors (MKIs) with anti-RET activity in RET-altered patients appears limited, calling into question the therapeutic potential of targeting RET. LOXO-292 is a selective RET inhibitor designed to inhibit diverse RET fusions, activating mutations and acquired resistance mutations. Patients and methods: Potent anti-RET activity, high selectivity, and central nervous system coverage were confirmed preclinically using a variety of in vitro and in vivo RET-dependent tumor models. Due to clinical urgency, two patients with RETaltered, MKI-resistant cancers were treated with LOXO-292, utilizing rapid dose-titration guided by real-time pharmacokinetic assessments to achieve meaningful clinical exposures safely and rapidly. Results: LOXO-292 demonstrated potent and selective anti-RET activity preclinically against human cancer cell lines harboring endogenous RET gene alterations; cells engineered to express a KIF5B-RET fusion protein -/+ the RET V804M gatekeeper resistance mutation or the common RET activating mutation M918T; and RET-altered human cancer cell line and patient-derived xenografts, including a patient-derived RET fusion-positive xenograft injected orthotopically into the brain. A patient with RET M918T-mutant medullary thyroid cancer metastatic to the liver and an acquired RET V804M gatekeeper resistance mutation, previously treated with six MKI regimens, experienced rapid reductions in tumor calcitonin, CEA and cell-free DNA, resolution of painful hepatomegaly and tumor-related diarrhea and a confirmed tumor response. A second patient with KIF5B-RET fusionpositive lung cancer, acquired resistance to alectinib and symptomatic brain metastases experienced a dramatic response in the brain, and her symptoms resolved. Conclusions: These results provide proof-of-concept of the clinical actionability of RET alterations, and identify selective RET inhibition by LOXO-292 as a promising treatment in heavily pretreated, multikinase inhibitor-experienced patients with diverse RET-altered tumors.",

keywords = "RET, TKI, gatekeeper, multiknase inhibitor, targeted kinase inhibitor",

author = "V. Subbiah and V. Velcheti and Tuch, {B. B.} and K. Ebata and Busaidy, {N. L.} and Cabanillas, {M. E.} and Wirth, {L. J.} and S. Stock and S. Smith and V. Lauriault and S. Corsi-Travali and D. Henry and M. Burkard and R. Hamor and K. Bouhana and S. Winski and Wallace, {R. D.} and D. Hartley and S. Rhodes and M. Reddy and Brandhuber, {B. J.} and S. Andrews and Rothenberg, {S. M.} and A. Drilon",

note = "Funding Information: The University of Texas MD Anderson Cancer Center is supported by the National Institutes of Health Cancer Center Support Grant CA016672. The University of Texas MD Anderson Cancer Center clinical trials program is supported in part by Cancer Prevention Research Institute of Texas Grant RP110584 and National Center for Advancing Translational Sciences Grant UL1 TR000371 (Center for Clinical and Translational Sciences). Publisher Copyright: {\textcopyright} The Author(s) 2018.",

year = "2018",

month = aug,

doi = "10.1093/annonc/mdy137",

language = "English (US)",

volume = "29",

pages = "1869--1876",

journal = "Annals of Oncology",

issn = "0923-7534",

publisher = "Oxford University Press",

number = "8",

}

TY - JOUR

T1 - Selective RET kinase inhibition for patients with RET-altered cancers

AU - Subbiah, V.

AU - Velcheti, V.

AU - Tuch, B. B.

AU - Ebata, K.

AU - Busaidy, N. L.

AU - Cabanillas, M. E.

AU - Wirth, L. J.

AU - Stock, S.

AU - Smith, S.

AU - Lauriault, V.

AU - Corsi-Travali, S.

AU - Henry, D.

AU - Burkard, M.

AU - Hamor, R.

AU - Bouhana, K.

AU - Winski, S.

AU - Wallace, R. D.

AU - Hartley, D.

AU - Rhodes, S.

AU - Reddy, M.

AU - Brandhuber, B. J.

AU - Andrews, S.

AU - Rothenberg, S. M.

AU - Drilon, A.

N1 - Funding Information: The University of Texas MD Anderson Cancer Center is supported by the National Institutes of Health Cancer Center Support Grant CA016672. The University of Texas MD Anderson Cancer Center clinical trials program is supported in part by Cancer Prevention Research Institute of Texas Grant RP110584 and National Center for Advancing Translational Sciences Grant UL1 TR000371 (Center for Clinical and Translational Sciences). Publisher Copyright: © The Author(s) 2018.

PY - 2018/8

Y1 - 2018/8

N2 - Background: Alterations involving the RET kinase are implicated in the pathogenesis of lung, thyroid and other cancers. However, the clinical activity of multikinase inhibitors (MKIs) with anti-RET activity in RET-altered patients appears limited, calling into question the therapeutic potential of targeting RET. LOXO-292 is a selective RET inhibitor designed to inhibit diverse RET fusions, activating mutations and acquired resistance mutations. Patients and methods: Potent anti-RET activity, high selectivity, and central nervous system coverage were confirmed preclinically using a variety of in vitro and in vivo RET-dependent tumor models. Due to clinical urgency, two patients with RETaltered, MKI-resistant cancers were treated with LOXO-292, utilizing rapid dose-titration guided by real-time pharmacokinetic assessments to achieve meaningful clinical exposures safely and rapidly. Results: LOXO-292 demonstrated potent and selective anti-RET activity preclinically against human cancer cell lines harboring endogenous RET gene alterations; cells engineered to express a KIF5B-RET fusion protein -/+ the RET V804M gatekeeper resistance mutation or the common RET activating mutation M918T; and RET-altered human cancer cell line and patient-derived xenografts, including a patient-derived RET fusion-positive xenograft injected orthotopically into the brain. A patient with RET M918T-mutant medullary thyroid cancer metastatic to the liver and an acquired RET V804M gatekeeper resistance mutation, previously treated with six MKI regimens, experienced rapid reductions in tumor calcitonin, CEA and cell-free DNA, resolution of painful hepatomegaly and tumor-related diarrhea and a confirmed tumor response. A second patient with KIF5B-RET fusionpositive lung cancer, acquired resistance to alectinib and symptomatic brain metastases experienced a dramatic response in the brain, and her symptoms resolved. Conclusions: These results provide proof-of-concept of the clinical actionability of RET alterations, and identify selective RET inhibition by LOXO-292 as a promising treatment in heavily pretreated, multikinase inhibitor-experienced patients with diverse RET-altered tumors.

AB - Background: Alterations involving the RET kinase are implicated in the pathogenesis of lung, thyroid and other cancers. However, the clinical activity of multikinase inhibitors (MKIs) with anti-RET activity in RET-altered patients appears limited, calling into question the therapeutic potential of targeting RET. LOXO-292 is a selective RET inhibitor designed to inhibit diverse RET fusions, activating mutations and acquired resistance mutations. Patients and methods: Potent anti-RET activity, high selectivity, and central nervous system coverage were confirmed preclinically using a variety of in vitro and in vivo RET-dependent tumor models. Due to clinical urgency, two patients with RETaltered, MKI-resistant cancers were treated with LOXO-292, utilizing rapid dose-titration guided by real-time pharmacokinetic assessments to achieve meaningful clinical exposures safely and rapidly. Results: LOXO-292 demonstrated potent and selective anti-RET activity preclinically against human cancer cell lines harboring endogenous RET gene alterations; cells engineered to express a KIF5B-RET fusion protein -/+ the RET V804M gatekeeper resistance mutation or the common RET activating mutation M918T; and RET-altered human cancer cell line and patient-derived xenografts, including a patient-derived RET fusion-positive xenograft injected orthotopically into the brain. A patient with RET M918T-mutant medullary thyroid cancer metastatic to the liver and an acquired RET V804M gatekeeper resistance mutation, previously treated with six MKI regimens, experienced rapid reductions in tumor calcitonin, CEA and cell-free DNA, resolution of painful hepatomegaly and tumor-related diarrhea and a confirmed tumor response. A second patient with KIF5B-RET fusionpositive lung cancer, acquired resistance to alectinib and symptomatic brain metastases experienced a dramatic response in the brain, and her symptoms resolved. Conclusions: These results provide proof-of-concept of the clinical actionability of RET alterations, and identify selective RET inhibition by LOXO-292 as a promising treatment in heavily pretreated, multikinase inhibitor-experienced patients with diverse RET-altered tumors.

KW - RET

KW - TKI

KW - gatekeeper

KW - multiknase inhibitor

KW - targeted kinase inhibitor

UR - http://www.scopus.com/inward/record.url?scp=85054935868&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85054935868&partnerID=8YFLogxK

U2 - 10.1093/annonc/mdy137

DO - 10.1093/annonc/mdy137

M3 - Article

C2 - 29912274

AN - SCOPUS:85054935868

SN - 0923-7534

VL - 29

SP - 1869

EP - 1876

JO - Annals of Oncology

JF - Annals of Oncology

IS - 8

ER -

Selective RET kinase inhibition for patients with RET-altered cancers

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this