Cutaneous adverse effects of targeted therapies: Part I: Inhibitors of the cellular membrane

James B. Macdonald; Brooke Macdonald; Loren E. Golitz; Patricia LoRusso; Aleksandar Sekulic

doi:10.1016/j.jaad.2014.07.032

Cutaneous adverse effects of targeted therapies: Part I: Inhibitors of the cellular membrane

James B. Macdonald, Brooke Macdonald, Loren E. Golitz, Patricia LoRusso, Aleksandar Sekulic

Dermatology

Research output: Contribution to journal › Review article › peer-review

122 Scopus citations

Abstract

There has been a rapid emergence of numerous targeted agents in the oncology community in the last decade. This exciting paradigm shift in drug development lends promise for the future of individualized medicine. Given the pace of development and clinical deployment of targeted agents with novel mechanisms of action, dermatology providers may not be familiar with the full spectrum of associated skin-related toxicities. Cutaneous adverse effects are among the most frequently observed toxicities with many targeted agents, and their intensity can be dose-limiting or lead to therapy discontinuation. In light of the often life-saving nature of emerging oncotherapeutics, it is critical that dermatologists both understand the mechanisms and recognize clinical signs and symptoms of such toxicities in order to provide effective clinical management. Part I of this continuing medical education article will review in detail the potential skin-related adverse sequelae, the frequency of occurrence, and the implications associated with on- and off-target cutaneous toxicities of inhibitors acting at the cell membrane level, chiefly inhibitors of epidermal growth factor receptor, KIT, and BCR-ABL, angiogenesis, and multikinase inhibitors.

Original language	English (US)
Pages (from-to)	203-218
Number of pages	16
Journal	Journal of the American Academy of Dermatology
Volume	72
Issue number	2
DOIs	https://doi.org/10.1016/j.jaad.2014.07.032
State	Published - 2015

Keywords

Adverse sequelae
Alopecia
Antiangiogenic agents
Anticancer
BCR-ABL
Bevacizumab
Cancer treatment
Canertinib
Cetuximab
Chemotherapy
Cutaneous adverse effects
Dasatinib
Dermatologic toxicities
Disturbed wound healing
Drug eruption
Drug rash
Drug reaction
Dry skin
Dual kinase inhibitors
Epidermal growth factor receptor inhibitors
Erlotinib
Gefitinib
Genital rash
HER2
Hyperkeratotic handefoot skin reaction
Imatinib
KIT
Lapatinib
Macular eruption
Monoclonal antibodies
Morbilliform
Mucocutaneous hemorrhage
Mucositis
Multikinase inhibitors
Nilotinib
Panitumumab
Papulopustular eruption
Paronychia
Pazopanib
Photosensitivity
Pigment changes
Platelet-derived growth factor receptor
Ranibizumab
Side effects
Small molecule
Sorafenib
Stomatitis
Sunitinib
Supportive oncodermatology
Targeted therapy
Toxic erythema
Tyrosine kinase inhibitors
Vandetanib
Vascular endothelial growth factor
Xerosis
erbB receptor

ASJC Scopus subject areas

Dermatology

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10.1016/j.jaad.2014.07.032

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title = "Cutaneous adverse effects of targeted therapies: Part I: Inhibitors of the cellular membrane",

abstract = "There has been a rapid emergence of numerous targeted agents in the oncology community in the last decade. This exciting paradigm shift in drug development lends promise for the future of individualized medicine. Given the pace of development and clinical deployment of targeted agents with novel mechanisms of action, dermatology providers may not be familiar with the full spectrum of associated skin-related toxicities. Cutaneous adverse effects are among the most frequently observed toxicities with many targeted agents, and their intensity can be dose-limiting or lead to therapy discontinuation. In light of the often life-saving nature of emerging oncotherapeutics, it is critical that dermatologists both understand the mechanisms and recognize clinical signs and symptoms of such toxicities in order to provide effective clinical management. Part I of this continuing medical education article will review in detail the potential skin-related adverse sequelae, the frequency of occurrence, and the implications associated with on- and off-target cutaneous toxicities of inhibitors acting at the cell membrane level, chiefly inhibitors of epidermal growth factor receptor, KIT, and BCR-ABL, angiogenesis, and multikinase inhibitors.",

keywords = "Adverse sequelae, Alopecia, Antiangiogenic agents, Anticancer, BCR-ABL, Bevacizumab, Cancer treatment, Canertinib, Cetuximab, Chemotherapy, Cutaneous adverse effects, Dasatinib, Dermatologic toxicities, Disturbed wound healing, Drug eruption, Drug rash, Drug reaction, Dry skin, Dual kinase inhibitors, Epidermal growth factor receptor inhibitors, Erlotinib, Gefitinib, Genital rash, HER2, Hyperkeratotic handefoot skin reaction, Imatinib, KIT, Lapatinib, Macular eruption, Monoclonal antibodies, Morbilliform, Mucocutaneous hemorrhage, Mucositis, Multikinase inhibitors, Nilotinib, Panitumumab, Papulopustular eruption, Paronychia, Pazopanib, Photosensitivity, Pigment changes, Platelet-derived growth factor receptor, Ranibizumab, Side effects, Small molecule, Sorafenib, Stomatitis, Sunitinib, Supportive oncodermatology, Targeted therapy, Toxic erythema, Tyrosine kinase inhibitors, Vandetanib, Vascular endothelial growth factor, Xerosis, erbB receptor",

author = "Macdonald, {James B.} and Brooke Macdonald and Golitz, {Loren E.} and Patricia LoRusso and Aleksandar Sekulic",

note = "Publisher Copyright: {\textcopyright} 2014 by the American Academy of Dermatology, Inc.",

year = "2015",

doi = "10.1016/j.jaad.2014.07.032",

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T2 - Part I: Inhibitors of the cellular membrane

AU - Macdonald, James B.

AU - Macdonald, Brooke

AU - Golitz, Loren E.

AU - LoRusso, Patricia

AU - Sekulic, Aleksandar

PY - 2015

Y1 - 2015

N2 - There has been a rapid emergence of numerous targeted agents in the oncology community in the last decade. This exciting paradigm shift in drug development lends promise for the future of individualized medicine. Given the pace of development and clinical deployment of targeted agents with novel mechanisms of action, dermatology providers may not be familiar with the full spectrum of associated skin-related toxicities. Cutaneous adverse effects are among the most frequently observed toxicities with many targeted agents, and their intensity can be dose-limiting or lead to therapy discontinuation. In light of the often life-saving nature of emerging oncotherapeutics, it is critical that dermatologists both understand the mechanisms and recognize clinical signs and symptoms of such toxicities in order to provide effective clinical management. Part I of this continuing medical education article will review in detail the potential skin-related adverse sequelae, the frequency of occurrence, and the implications associated with on- and off-target cutaneous toxicities of inhibitors acting at the cell membrane level, chiefly inhibitors of epidermal growth factor receptor, KIT, and BCR-ABL, angiogenesis, and multikinase inhibitors.

AB - There has been a rapid emergence of numerous targeted agents in the oncology community in the last decade. This exciting paradigm shift in drug development lends promise for the future of individualized medicine. Given the pace of development and clinical deployment of targeted agents with novel mechanisms of action, dermatology providers may not be familiar with the full spectrum of associated skin-related toxicities. Cutaneous adverse effects are among the most frequently observed toxicities with many targeted agents, and their intensity can be dose-limiting or lead to therapy discontinuation. In light of the often life-saving nature of emerging oncotherapeutics, it is critical that dermatologists both understand the mechanisms and recognize clinical signs and symptoms of such toxicities in order to provide effective clinical management. Part I of this continuing medical education article will review in detail the potential skin-related adverse sequelae, the frequency of occurrence, and the implications associated with on- and off-target cutaneous toxicities of inhibitors acting at the cell membrane level, chiefly inhibitors of epidermal growth factor receptor, KIT, and BCR-ABL, angiogenesis, and multikinase inhibitors.

KW - Adverse sequelae

KW - Alopecia

KW - Antiangiogenic agents

KW - Anticancer

KW - BCR-ABL

KW - Bevacizumab

KW - Cancer treatment

KW - Canertinib

KW - Cetuximab

KW - Chemotherapy

KW - Cutaneous adverse effects

KW - Dasatinib

KW - Dermatologic toxicities

KW - Disturbed wound healing

KW - Drug eruption

KW - Drug rash

KW - Drug reaction

KW - Dry skin

KW - Dual kinase inhibitors

KW - Epidermal growth factor receptor inhibitors

KW - Erlotinib

KW - Gefitinib

KW - Genital rash

KW - HER2

KW - Hyperkeratotic handefoot skin reaction

KW - Imatinib

KW - KIT

KW - Lapatinib

KW - Macular eruption

KW - Monoclonal antibodies

KW - Morbilliform

KW - Mucocutaneous hemorrhage

KW - Mucositis

KW - Multikinase inhibitors

KW - Nilotinib

KW - Panitumumab

KW - Papulopustular eruption

KW - Paronychia

KW - Pazopanib

KW - Photosensitivity

KW - Pigment changes

KW - Platelet-derived growth factor receptor

KW - Ranibizumab

KW - Side effects

KW - Small molecule

KW - Sorafenib

KW - Stomatitis

KW - Sunitinib

KW - Supportive oncodermatology

KW - Targeted therapy

KW - Toxic erythema

KW - Tyrosine kinase inhibitors

KW - Vandetanib

KW - Vascular endothelial growth factor

KW - Xerosis

KW - erbB receptor

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DO - 10.1016/j.jaad.2014.07.032

M3 - Review article

C2 - 25592338

AN - SCOPUS:84922516101

SN - 0190-9622

VL - 72

SP - 203

EP - 218

JO - Journal of the American Academy of Dermatology

JF - Journal of the American Academy of Dermatology

IS - 2

ER -

Cutaneous adverse effects of targeted therapies: Part I: Inhibitors of the cellular membrane

Abstract

Keywords

ASJC Scopus subject areas

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