Epidermal Growth Factor Receptor (EGFR) Inhibitor-Induced Rash: A Consecutive Patient Series that Illustrates the Need for Rigorous Palliative Trials

Solomon, Benjamin; Jatoi, Aminah

doi:10.1089/jpm.2010.0258

Cited by 10 publications

(8 citation statements)

References 13 publications

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“…argeted therapies in particular epidermal growth factor (EGFR)-inhibitors have emerged as the primary therapy in advanced solid tumor malignancies including colorectal, pancreas, head and neck cancers, and non-small cell lung carcinoma because of improvement in survival with overall favorable side effect profile. 1,2 EGFR-inhibitors include small molecule tyrosine kinase inhibitors (TKIs) such as gefitinib, erlotinib, and lapatinib, as well as monoclonal antibodies such as cetuximab and panitumumab. 3,4,5 However, 50-90% of patients treated with EGFR-inhibitors develop a follicular or acneiform rash, which can be symptomatic and source of psychosocial distress, negatively impacting quality of life.…”

Section: Introduction Tmentioning

confidence: 99%

“…3,4,5 However, 50-90% of patients treated with EGFR-inhibitors develop a follicular or acneiform rash, which can be symptomatic and source of psychosocial distress, negatively impacting quality of life. 1,2,3 The pathogenesis of this rash is thought to be due to EGFR inhibition preventing keratinocyte migration, inducing keratinocyte apoptosis, and modulating cytokine release, which leads to the influx of inflammatory cells in the epidermis and dermis. 2,6 The epidermis becomes thin leading to skin atrophy and xerosis, and extensive follicular involvement can lead to scarring alopecia.…”

Section: Introduction Tmentioning

confidence: 99%

“…4 Areas with the highest follicle and sebaceous gland density, including the head and neck, chest, and back, are most frequently involved. 1,4 As this acneiform rash is a well-recognized cutaneous toxicity of EGFR-inhibitors, a treatment algorithm has been proposed for management based on severity. However, this algorithm does not account for biologic differences in skin in patients of different races and ethnicities.…”

Section: Introduction Tmentioning

confidence: 99%

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Cutaneous Manifestations of EGFR-Inhibitors in African Americans and Treatment Considerations

Geisler¹,

Noor²

2020

JDD

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Epidermal growth factor (EGFR)-inhibitors have emerged as the primary therapy in advanced solid tumor malignancies because of improvement in survival with overall favorable side effect profile. However, 50-90% of patients treated with EGFR-inhibitors develop a follicular or acneiform rash, which can be symptomatic and source of psychosocial distress, negatively impacting quality of life. As this acneiform rash is a well-recognized cutaneous toxicity of EGFR-inhibitors, a treatment algorithm has been proposed for management based on severity. However, treatment options for EGFR-inhibitor induced rash may not be generalizable to African Americans whose differences in skin biology and sensitivity present pathophysiologic challenges. Herein, we present a case of an African American patient who developed this acneiform rash while on cetuximab. We also review the few cases that have been reported in the literature of EGFR-inhibitor rash in African Americans, highlighting important management considerations in this patient population.

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Section: Introduction Tmentioning

confidence: 99%

Section: Introduction Tmentioning

confidence: 99%

Section: Introduction Tmentioning

confidence: 99%

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Cutaneous Manifestations of EGFR-Inhibitors in African Americans and Treatment Considerations

Geisler¹,

Noor²

2020

JDD

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“…Newer and more-intensive therapies have resulted in better disease control and the emergence of cancer as a chronic disease [24–28]. However, these newer therapies are sometimes associated with unexpected side effects that clinicians are not prepared to manage [29–33]. Furthermore, newer therapies are often administered orally and may require long-term use to control cancer.…”

Section: Symptom Assessment In Cancer Researchmentioning

confidence: 99%

Measuring symptoms as a critical component of drug development and evaluation in hematological diseases

Williams

Yücel

Cortés

et al. 2013

Clinical Investigation

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With the rapid development of new therapies for patients with hematological malignancies, there is an increasing need for patient report of symptom status during all phases of drug testing. The patient’s perspective on new treatments reflects treatment tolerability as well as symptom benefit, and may assist patients and clinicians in choosing treatments. Inclusion of patient-reported outcomes, more common in solid-tumor than hematological trials, provides early information about symptoms to guide decisions about appropriate dosing and supportive care needs. We provide a historical overview of the use of patient-reported outcomes and symptom assessment in solid-tumor and hematological drug development, and offer recommendations about methodological issues in the monitoring of symptoms in the drug development process in hematological clinical trials.

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“…Radiation therapy is associated with increased fatigue and uncomfortable skin reactions (Bray, Simmons, Wolfson, & Nouri, 2016). Targeted therapies such as those that inhibit the epidermal growth factor receptor (EGFR) can cause an itchy, painful rash (Lacouture et al, 2011; Solomon & Jatoi, 2011; Wickersham et al, 2014) and diarrhea. Finally, the stress response associated with living with cancer can lead to chronic activation of the hypothalamic–pituitary–adrenal and sympathetic–adrenal–medullary axes, ultimately leading to a dysfunctional inflammatory response and elevated anxiety, depression, and pain (Subnis, Starkweather, McCain, & Brown, 2014).…”

Section: Introductionmentioning

confidence: 99%

Conducting Biobehavioral Research in Patients With Advanced Cancer: Recruitment Challenges and Solutions

Gilbertson‐White

Bohr

Wickersham

2017

Biological Research For Nursing

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Despite significant advances in cancer treatment and symptom management interventions over the last decade, patients continue to struggle with cancer-related symptoms. Adequate baseline and longitudinal data are crucial for designing interventions to improve patient quality of life and reduce symptom burden; however, recruitment of patients with advanced cancer in longitudinal research is difficult. Our purpose is to describe challenges and solutions to recruitment of patients with advanced cancer in two biobehavioral research studies examining cancer-related symptoms. Study 1: Symptom data and peripheral blood for markers of inflammation were collected from newly diagnosed patients receiving chemotherapy on the first day of therapy and every 3–4 weeks for up to 6 months. Study 2: Symptom data, blood, and skin biopsies were collected from cancer patients taking epidermal growth factor receptor inhibitors at specific time points over 4 months. Screening and recruitment results for both studies are summarized. Timing informed consent with baseline data collection prior to treatment initiation was a significant recruitment challenge for both the studies. Possible solutions include tailoring recruitment to fit clinic needs, increasing research staff availability during clinic hours, and adding recruitment sites. Identifying solutions to these challenges will permit the conduct of studies that may lead to identification of factors contributing to variability in symptoms and development of tailored patient interventions for patients with advanced cancer.

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Epidermal Growth Factor Receptor (EGFR) Inhibitor-Induced Rash: A Consecutive Patient Series that Illustrates the Need for Rigorous Palliative Trials

Cited by 10 publications

References 13 publications

Cutaneous Manifestations of EGFR-Inhibitors in African Americans and Treatment Considerations

Cutaneous Manifestations of EGFR-Inhibitors in African Americans and Treatment Considerations

Measuring symptoms as a critical component of drug development and evaluation in hematological diseases

Conducting Biobehavioral Research in Patients With Advanced Cancer: Recruitment Challenges and Solutions

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