Characterization of on-target adverse events caused by TRK inhibitor therapy

D. Liu; J. Flory; A. Lin; M. Offin; C. J. Falcon; Y. R. Murciano-Goroff; E. Rosen; R. Guo; E. Basu; B. T. Li; J. J. Harding; G. Iyer; K. Jhaveri; M. M. Gounder; N. N. Shukla; S. S. Roberts; J. Glade-Bender; L. Kaplanis; A. Schram; D. M. Hyman; A. Drilon

doi:10.1016/j.annonc.2020.05.006

Characterization of on-target adverse events caused by TRK inhibitor therapy

D. Liu, J. Flory, A. Lin, M. Offin, C. J. Falcon, Y. R. Murciano-Goroff, E. Rosen, R. Guo, E. Basu, B. T. Li, J. J. Harding, G. Iyer, K. Jhaveri, M. M. Gounder, N. N. Shukla, S. S. Roberts, J. Glade-Bender, L. Kaplanis, A. Schram, D. M. HymanA. Drilon

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

38 Scopus citations

Abstract

Background: The tropomyosin receptor kinase (TRK) pathway controls appetite, balance, and pain sensitivity. While these functions are reflected in the on-target adverse events (AEs) observed with TRK inhibition, these AEs remain under-recognized, and pain upon drug withdrawal has not previously been reported. As TRK inhibitors are approved by multiple regulatory agencies for TRK or ROS1 fusion-positive cancers, characterizing these AEs and corresponding management strategies is crucial. Patients and methods: Patients with advanced or unresectable solid tumors treated with a TRK inhibitor were retrospectively identified in a search of clinical databases. Among these patients, the frequency, severity, duration, and management outcomes of AEs including weight gain, dizziness or ataxia, and withdrawal pain were characterized. Results: Ninety-six patients with 15 unique cancer histologies treated with a TRK inhibitor were identified. Weight gain was observed in 53% [95% confidence interval (CI), 43%–62%] of patients and increased with time on TRK inhibition. Pharmacologic intervention, most commonly with glucagon-like peptide 1 analogs or metformin, appeared to result in stabilization or loss of weight. Dizziness, with or without ataxia, was observed in 41% (95% CI, 31%–51%) of patients with a median time to onset of 2 weeks (range, 3 days to 16 months). TRK inhibitor dose reduction was the most effective intervention for dizziness. Pain upon temporary or permanent TRK inhibitor discontinuation was observed in 35% (95% CI, 24%–46%) of patients; this was more common with longer TRK inhibitor use. TRK inhibitor reinitiation was the most effective intervention for withdrawal pain. Conclusions: TRK inhibition-related AEs including weight gain, dizziness, and withdrawal pain occur in a substantial proportion of patients receiving TRK inhibitors. This safety profile is unique relative to other anticancer therapies and warrants careful monitoring. These on-target toxicities are manageable with pharmacologic intervention and dose modification.

Original language	English (US)
Pages (from-to)	1207-1215
Number of pages	9
Journal	Annals of Oncology
Volume	31
Issue number	9
DOIs	https://doi.org/10.1016/j.annonc.2020.05.006
State	Published - Sep 2020
Externally published	Yes

Keywords

NTRK fusion
TRK inhibitors
toxicity management

ASJC Scopus subject areas

Hematology
Oncology

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10.1016/j.annonc.2020.05.006

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Liu, D., Flory, J., Lin, A., Offin, M., Falcon, C. J., Murciano-Goroff, Y. R., Rosen, E., Guo, R., Basu, E., Li, B. T., Harding, J. J., Iyer, G., Jhaveri, K., Gounder, M. M., Shukla, N. N., Roberts, S. S., Glade-Bender, J., Kaplanis, L., Schram, A., ... Drilon, A. (2020). Characterization of on-target adverse events caused by TRK inhibitor therapy. Annals of Oncology, 31(9), 1207-1215. https://doi.org/10.1016/j.annonc.2020.05.006

Liu, D, Flory, J, Lin, A, Offin, M, Falcon, CJ, Murciano-Goroff, YR, Rosen, E, Guo, R, Basu, E, Li, BT, Harding, JJ, Iyer, G, Jhaveri, K, Gounder, MM, Shukla, NN, Roberts, SS, Glade-Bender, J, Kaplanis, L, Schram, A, Hyman, DM & Drilon, A 2020, 'Characterization of on-target adverse events caused by TRK inhibitor therapy', Annals of Oncology, vol. 31, no. 9, pp. 1207-1215. https://doi.org/10.1016/j.annonc.2020.05.006

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title = "Characterization of on-target adverse events caused by TRK inhibitor therapy",

abstract = "Background: The tropomyosin receptor kinase (TRK) pathway controls appetite, balance, and pain sensitivity. While these functions are reflected in the on-target adverse events (AEs) observed with TRK inhibition, these AEs remain under-recognized, and pain upon drug withdrawal has not previously been reported. As TRK inhibitors are approved by multiple regulatory agencies for TRK or ROS1 fusion-positive cancers, characterizing these AEs and corresponding management strategies is crucial. Patients and methods: Patients with advanced or unresectable solid tumors treated with a TRK inhibitor were retrospectively identified in a search of clinical databases. Among these patients, the frequency, severity, duration, and management outcomes of AEs including weight gain, dizziness or ataxia, and withdrawal pain were characterized. Results: Ninety-six patients with 15 unique cancer histologies treated with a TRK inhibitor were identified. Weight gain was observed in 53% [95% confidence interval (CI), 43%–62%] of patients and increased with time on TRK inhibition. Pharmacologic intervention, most commonly with glucagon-like peptide 1 analogs or metformin, appeared to result in stabilization or loss of weight. Dizziness, with or without ataxia, was observed in 41% (95% CI, 31%–51%) of patients with a median time to onset of 2 weeks (range, 3 days to 16 months). TRK inhibitor dose reduction was the most effective intervention for dizziness. Pain upon temporary or permanent TRK inhibitor discontinuation was observed in 35% (95% CI, 24%–46%) of patients; this was more common with longer TRK inhibitor use. TRK inhibitor reinitiation was the most effective intervention for withdrawal pain. Conclusions: TRK inhibition-related AEs including weight gain, dizziness, and withdrawal pain occur in a substantial proportion of patients receiving TRK inhibitors. This safety profile is unique relative to other anticancer therapies and warrants careful monitoring. These on-target toxicities are manageable with pharmacologic intervention and dose modification.",

keywords = "NTRK fusion, TRK inhibitors, toxicity management",

author = "D. Liu and J. Flory and A. Lin and M. Offin and Falcon, {C. J.} and Murciano-Goroff, {Y. R.} and E. Rosen and R. Guo and E. Basu and Li, {B. T.} and Harding, {J. J.} and G. Iyer and K. Jhaveri and Gounder, {M. M.} and Shukla, {N. N.} and Roberts, {S. S.} and J. Glade-Bender and L. Kaplanis and A. Schram and Hyman, {D. M.} and A. Drilon",

note = "Publisher Copyright: {\textcopyright} 2020 European Society for Medical Oncology",

year = "2020",

month = sep,

doi = "10.1016/j.annonc.2020.05.006",

language = "English (US)",

volume = "31",

pages = "1207--1215",

journal = "Annals of Oncology",

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number = "9",

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TY - JOUR

T1 - Characterization of on-target adverse events caused by TRK inhibitor therapy

AU - Liu, D.

AU - Flory, J.

AU - Lin, A.

AU - Offin, M.

AU - Falcon, C. J.

AU - Murciano-Goroff, Y. R.

AU - Rosen, E.

AU - Guo, R.

AU - Basu, E.

AU - Li, B. T.

AU - Harding, J. J.

AU - Iyer, G.

AU - Jhaveri, K.

AU - Gounder, M. M.

AU - Shukla, N. N.

AU - Roberts, S. S.

AU - Glade-Bender, J.

AU - Kaplanis, L.

AU - Schram, A.

AU - Hyman, D. M.

AU - Drilon, A.

PY - 2020/9

Y1 - 2020/9

N2 - Background: The tropomyosin receptor kinase (TRK) pathway controls appetite, balance, and pain sensitivity. While these functions are reflected in the on-target adverse events (AEs) observed with TRK inhibition, these AEs remain under-recognized, and pain upon drug withdrawal has not previously been reported. As TRK inhibitors are approved by multiple regulatory agencies for TRK or ROS1 fusion-positive cancers, characterizing these AEs and corresponding management strategies is crucial. Patients and methods: Patients with advanced or unresectable solid tumors treated with a TRK inhibitor were retrospectively identified in a search of clinical databases. Among these patients, the frequency, severity, duration, and management outcomes of AEs including weight gain, dizziness or ataxia, and withdrawal pain were characterized. Results: Ninety-six patients with 15 unique cancer histologies treated with a TRK inhibitor were identified. Weight gain was observed in 53% [95% confidence interval (CI), 43%–62%] of patients and increased with time on TRK inhibition. Pharmacologic intervention, most commonly with glucagon-like peptide 1 analogs or metformin, appeared to result in stabilization or loss of weight. Dizziness, with or without ataxia, was observed in 41% (95% CI, 31%–51%) of patients with a median time to onset of 2 weeks (range, 3 days to 16 months). TRK inhibitor dose reduction was the most effective intervention for dizziness. Pain upon temporary or permanent TRK inhibitor discontinuation was observed in 35% (95% CI, 24%–46%) of patients; this was more common with longer TRK inhibitor use. TRK inhibitor reinitiation was the most effective intervention for withdrawal pain. Conclusions: TRK inhibition-related AEs including weight gain, dizziness, and withdrawal pain occur in a substantial proportion of patients receiving TRK inhibitors. This safety profile is unique relative to other anticancer therapies and warrants careful monitoring. These on-target toxicities are manageable with pharmacologic intervention and dose modification.

AB - Background: The tropomyosin receptor kinase (TRK) pathway controls appetite, balance, and pain sensitivity. While these functions are reflected in the on-target adverse events (AEs) observed with TRK inhibition, these AEs remain under-recognized, and pain upon drug withdrawal has not previously been reported. As TRK inhibitors are approved by multiple regulatory agencies for TRK or ROS1 fusion-positive cancers, characterizing these AEs and corresponding management strategies is crucial. Patients and methods: Patients with advanced or unresectable solid tumors treated with a TRK inhibitor were retrospectively identified in a search of clinical databases. Among these patients, the frequency, severity, duration, and management outcomes of AEs including weight gain, dizziness or ataxia, and withdrawal pain were characterized. Results: Ninety-six patients with 15 unique cancer histologies treated with a TRK inhibitor were identified. Weight gain was observed in 53% [95% confidence interval (CI), 43%–62%] of patients and increased with time on TRK inhibition. Pharmacologic intervention, most commonly with glucagon-like peptide 1 analogs or metformin, appeared to result in stabilization or loss of weight. Dizziness, with or without ataxia, was observed in 41% (95% CI, 31%–51%) of patients with a median time to onset of 2 weeks (range, 3 days to 16 months). TRK inhibitor dose reduction was the most effective intervention for dizziness. Pain upon temporary or permanent TRK inhibitor discontinuation was observed in 35% (95% CI, 24%–46%) of patients; this was more common with longer TRK inhibitor use. TRK inhibitor reinitiation was the most effective intervention for withdrawal pain. Conclusions: TRK inhibition-related AEs including weight gain, dizziness, and withdrawal pain occur in a substantial proportion of patients receiving TRK inhibitors. This safety profile is unique relative to other anticancer therapies and warrants careful monitoring. These on-target toxicities are manageable with pharmacologic intervention and dose modification.

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KW - TRK inhibitors

KW - toxicity management

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Characterization of on-target adverse events caused by TRK inhibitor therapy

Abstract

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