RS Bhangoo , TW Cheng , MM Petersen , CS Thorpe , TA DeWees , JD Anderson , CE Vargas , SH Patel , MY Halyard , SE Schild , WW Wong
{"title":"辐射回忆性皮炎:文献综述","authors":"RS Bhangoo , TW Cheng , MM Petersen , CS Thorpe , TA DeWees , JD Anderson , CE Vargas , SH Patel , MY Halyard , SE Schild , WW Wong","doi":"10.1053/j.seminoncol.2022.04.001","DOIUrl":null,"url":null,"abstract":"<div><h3>Purpose/Objectives</h3><p><span>Radiation recall dermatitis (RRD) is a skin reaction limited to an area of prior radiation triggered by the subsequent introduction of systemic therapy. To characterize RRD, we conducted a literature search, summarized RRD features, and compared the most common </span>drug classes implicated in this phenomenon.</p></div><div><h3>Materials/Methods</h3><p>PubMed, Embase<span>, Scopus<span>, Web of Science, and Cochrane DBSR databases were queried through July 1, 2019 using key words: radiation recall, RRD, and radiodermatitis (limited to humans and English language). Studies included case reports in which patients treated with radiotherapy were initiated on a new line of systemic therapy and subsequently developed a skin reaction in the irradiated area. RRD cases were organized by whether RRD occurred after a single drug or multiple drug administration.</span></span></p></div><div><h3>Results</h3><p><span><span>One-hundred fifteen studies representing 129 RRD cases (96 single-drug RRD, 33 multi-drug) were included. Sixty-three drugs were associated with RRD. Docetaxel (22) and </span>gemcitabine (18) were the two drugs most commonly associated with RRD. Breast cancer (69 cases) was the most commonly associated tumor type. For single-drug RRD, the median radiotherapy dose was 45.0 Gy (range, 30.0–63.2 Gy). The median time from radiotherapy to drug exposure, time from drug exposure to RRD and time to significant improvement was 8 weeks (range, 2–132 weeks), 5 days (range, 2–56 days), and 14 days (range, 7–49 days), respectively. Variables significantly associated with grade ≥2 toxicity were docetaxel (</span><em>P</em><span> = 0.04) and non-antifolate antimetabolite (</span><em>P</em><span> = 0.05). The only variable significantly associated with grade ≥3 toxicity was capecitabine (</span><em>P</em> = 0.04).</p></div><div><h3>Conclusions</h3><p>RRD is a complex toxicity that can occur after a wide range of radiotherapy doses and many different systemic agents. Most commonly, it presents in patients<span><span> diagnosed with breast cancer and after administration of a taxane or antimetabolite medication. RRD treatment generally consists of corticosteroids with consideration of antibiotics if </span>superinfection is suspected. Drug re-challenge may be considered after RRD if the initial reaction was of mild intensity.</span></p></div>","PeriodicalId":21750,"journal":{"name":"Seminars in oncology","volume":"49 2","pages":"Pages 152-159"},"PeriodicalIF":3.0000,"publicationDate":"2022-04-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"9","resultStr":"{\"title\":\"Radiation recall dermatitis: A review of the literature\",\"authors\":\"RS Bhangoo , TW Cheng , MM Petersen , CS Thorpe , TA DeWees , JD Anderson , CE Vargas , SH Patel , MY Halyard , SE Schild , WW Wong\",\"doi\":\"10.1053/j.seminoncol.2022.04.001\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<div><h3>Purpose/Objectives</h3><p><span>Radiation recall dermatitis (RRD) is a skin reaction limited to an area of prior radiation triggered by the subsequent introduction of systemic therapy. To characterize RRD, we conducted a literature search, summarized RRD features, and compared the most common </span>drug classes implicated in this phenomenon.</p></div><div><h3>Materials/Methods</h3><p>PubMed, Embase<span>, Scopus<span>, Web of Science, and Cochrane DBSR databases were queried through July 1, 2019 using key words: radiation recall, RRD, and radiodermatitis (limited to humans and English language). Studies included case reports in which patients treated with radiotherapy were initiated on a new line of systemic therapy and subsequently developed a skin reaction in the irradiated area. RRD cases were organized by whether RRD occurred after a single drug or multiple drug administration.</span></span></p></div><div><h3>Results</h3><p><span><span>One-hundred fifteen studies representing 129 RRD cases (96 single-drug RRD, 33 multi-drug) were included. Sixty-three drugs were associated with RRD. Docetaxel (22) and </span>gemcitabine (18) were the two drugs most commonly associated with RRD. Breast cancer (69 cases) was the most commonly associated tumor type. For single-drug RRD, the median radiotherapy dose was 45.0 Gy (range, 30.0–63.2 Gy). The median time from radiotherapy to drug exposure, time from drug exposure to RRD and time to significant improvement was 8 weeks (range, 2–132 weeks), 5 days (range, 2–56 days), and 14 days (range, 7–49 days), respectively. Variables significantly associated with grade ≥2 toxicity were docetaxel (</span><em>P</em><span> = 0.04) and non-antifolate antimetabolite (</span><em>P</em><span> = 0.05). The only variable significantly associated with grade ≥3 toxicity was capecitabine (</span><em>P</em> = 0.04).</p></div><div><h3>Conclusions</h3><p>RRD is a complex toxicity that can occur after a wide range of radiotherapy doses and many different systemic agents. Most commonly, it presents in patients<span><span> diagnosed with breast cancer and after administration of a taxane or antimetabolite medication. RRD treatment generally consists of corticosteroids with consideration of antibiotics if </span>superinfection is suspected. 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Radiation recall dermatitis: A review of the literature
Purpose/Objectives
Radiation recall dermatitis (RRD) is a skin reaction limited to an area of prior radiation triggered by the subsequent introduction of systemic therapy. To characterize RRD, we conducted a literature search, summarized RRD features, and compared the most common drug classes implicated in this phenomenon.
Materials/Methods
PubMed, Embase, Scopus, Web of Science, and Cochrane DBSR databases were queried through July 1, 2019 using key words: radiation recall, RRD, and radiodermatitis (limited to humans and English language). Studies included case reports in which patients treated with radiotherapy were initiated on a new line of systemic therapy and subsequently developed a skin reaction in the irradiated area. RRD cases were organized by whether RRD occurred after a single drug or multiple drug administration.
Results
One-hundred fifteen studies representing 129 RRD cases (96 single-drug RRD, 33 multi-drug) were included. Sixty-three drugs were associated with RRD. Docetaxel (22) and gemcitabine (18) were the two drugs most commonly associated with RRD. Breast cancer (69 cases) was the most commonly associated tumor type. For single-drug RRD, the median radiotherapy dose was 45.0 Gy (range, 30.0–63.2 Gy). The median time from radiotherapy to drug exposure, time from drug exposure to RRD and time to significant improvement was 8 weeks (range, 2–132 weeks), 5 days (range, 2–56 days), and 14 days (range, 7–49 days), respectively. Variables significantly associated with grade ≥2 toxicity were docetaxel (P = 0.04) and non-antifolate antimetabolite (P = 0.05). The only variable significantly associated with grade ≥3 toxicity was capecitabine (P = 0.04).
Conclusions
RRD is a complex toxicity that can occur after a wide range of radiotherapy doses and many different systemic agents. Most commonly, it presents in patients diagnosed with breast cancer and after administration of a taxane or antimetabolite medication. RRD treatment generally consists of corticosteroids with consideration of antibiotics if superinfection is suspected. Drug re-challenge may be considered after RRD if the initial reaction was of mild intensity.
期刊介绍:
Seminars in Oncology brings you current, authoritative, and practical reviews of developments in the etiology, diagnosis and management of cancer. Each issue examines topics of clinical importance, with an emphasis on providing both the basic knowledge needed to better understand a topic as well as evidence-based opinions from leaders in the field. Seminars in Oncology also seeks to be a venue for sharing a diversity of opinions including those that might be considered "outside the box". We welcome a healthy and respectful exchange of opinions and urge you to approach us with your insights as well as suggestions of topics that you deem worthy of coverage. By helping the reader understand the basic biology and the therapy of cancer as they learn the nuances from experts, all in a journal that encourages the exchange of ideas we aim to help move the treatment of cancer forward.
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