Pulmonary complications of immune checkpoint inhibitors in patients with nonsmall cell lung cancer

Cadranel, Jacques; Cañellas, A.; Matton, Lise; Darrason, Marie; Parrot, Antoine; Naccache, Jean‐Marc; Lavolé, A.; Ruppert, Anne-Marie; Fallet, Vincent

doi:10.1183/16000617.0058-2019

Cited by 79 publications

(89 citation statements)

References 152 publications

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“…There have also been case reports of sarcoid-like granulomatous changes associated with ICI, both on CT scan and lung biopsy, but these appear to be more common in patients with melanoma. 55,64 The histologic findings of ICI pneumonitis have not been well described as lung biopsy is not necessary to make the diagnosis of ICI pneumonitis, and biopsy results have been rarely reported in retrospective studies and case reports. Several studies have demonstrated increased lymphocyte proportion on BAL of patients with ICI pneumonitis.…”

Section: Radiographic and Histologic Featuresmentioning

confidence: 99%

Pulmonary toxicity of systemic lung cancer therapy

Long

Suresh

2020

Respirology

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Lung cancer is the leading cause of cancer-related deaths worldwide. As new therapies are developed, it is important to understand the pulmonary toxicities associated with systemic lung cancer therapies. Cytotoxic chemotherapy regimens for NSCLC often include taxanes. Pulmonary toxicity from taxanes presents as an ILD-type reaction characterized by increasing dyspnoea, dry cough, fever and bilateral pulmonary interstitial infiltrates. The incidence of taxane-induced pneumonitis is rare, and many patients respond to steroid therapy; however, fatal cases have been reported. Patients with NSCLC are routinely tested for the presence of tumour oncogenes to determine their candidacy for targeted therapies, such as TKI. EGFR-TKI can cause pneumonitis characterized by progressive dyspnoea and hypoxia. EGFR-TKIassociated ILD rarely presents as an AIP with rapidly progressive respiratory failure and high mortality rates. The most recent development in lung cancer therapy has been the discovery of immune checkpoint inhibitor (ICI). ICI pneumonitis has been increasingly recognized as a common complication of ICI therapy, with reported incidence as high as 19% in some clinical settings. Early-grade ICI pneumonitis may be asymptomatic; however, high-grade ICI pneumonitis can result in progressive dyspnoea, hypoxia and respiratory failure. ICI pneumonitis is unique in that only half of the patients will improve with steroid treatment, and mortality rates are high. As treatment of NSCLC evolves, providers must be able to recognize and respond to the development of drug-induced pulmonary toxicities.

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Section: Radiographic and Histologic Featuresmentioning

confidence: 99%

Pulmonary toxicity of systemic lung cancer therapy

Long

Suresh

2020

Respirology

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“…Also, the pre-existing autoimmune diseases seem not to predict complications [62;63]. The analysis of observations shows that lung fibrosis does not exclude immunotherapy [60]however the course of pulmonary complications may be accomplished by comorbidities. should be selected depending on the kind of ICI related toxicity and its clinical manifestation [79].…”

Section: Skin Toxicitymentioning

confidence: 99%

“…Bilateral distribution and localisation away from lung tumor are often observed[58]. Pleural effusion and mediastinal lymph nodes involvement are rare.The issue of CIP is non-infectious parenchymal inflammation and the COP, AIP or NSIP pattern was confirmed by histological examination, however the data are scanty[59].Sarcoid granulomatosis is a special kind of possible toxicity, however rare, it may involve extrapulmonary organs though[60].The differential diagnosis of new lung infiltrations in ICIs treated patients include tumor progression or pseudoprogression, pneumonia or pneumonitis. Thus, the full microbiological tests and histopathological examination of sputum/material from bronchoscopy is often needed and decisive.…”

mentioning

confidence: 99%

Immunotherapy of solid tumors: how safely treat the patients

Domagała‐Kulawik

Leszek

Owczarek

et al. 2020

Polish Archives of Internal Medicine

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Immunotherapy with immune checkpoint inhibitors (ICIs) was shown to improve survival of patients with solid tumors like: melanoma, renal carcinoma, non-small cell lung cancer, cutaneous carcinomas or head and neck carcinoma. However, a special type of ICIs toxicity is observed, namely non-infectious inflammation of different organs connected with autoimmunity known as immune related adverse events (irAEs). This non-infectious inflammation may affect different organs and systems as endocrine organs, the gastrointestinal tract, heart, skin and the nervous system. The lungs are also often involved and this condition is referred to as checkpoint inhibitor pneumonitis (CIP). ICIs toxicity is graded from 1 to 5 depending on the clinical course, the 5 grade being a fatal complication. Corticosteroids are the treatment of choice, generally with good efficacy. In some difficult cases, escalation of immunosuppression is required. The knowledge on irAEs should be promoted among clinicians of all specialties, nurses, patients and their families. The aim of this review is to present the wide spectrum of irAEs: clinical signs and symptoms, differential diagnosis, diagnostic procedures and treatment. The data are supported by our own clinical observations.

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“…According to a recent meta‐analysis of 125 clinical trials involving 20 128 patients, ICI adverse effects, such as severe myocarditis and pneumonitis, are challenging to diagnose and might not be treated promptly, finally affecting patients' survival 73 . Indeed, while in this class of patients, the general risk of bacteria and viral infections is low and not widely investigated in literature, 74 an ICI‐correlated pulmonary toxicity has been previously reported 75 . The overall incidence rate of ICI‐related pneumonitis ranges from 2.5% to 5% with anti‐PD‐1/PD‐L1 monotherapy from 7% to 10% with anti‐CTLA‐4 + anti‐PD‐1 combination therapy 76 .…”

Section: Onco‐dermatologymentioning

confidence: 99%

Systemic immunobiological, immunosuppressant, and oncologic agents for the treatment of dermatologic diseases during theSARS‐CoV‐2 (COVID‐19) pandemic emergency: A quick review for a quick consultation

Paolino

Mercuri

Bearzi

et al. 2020

Dermatologic Therapy

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The Precision Medicine Era has helped to better manage patients with immunological and oncological disease, improving the quality of life of this class of patients. Regarding the management of these patients and positivity to SARS-Cov2, currently, limited data is available and information is evolving. In this quick review we have analyzed the mechanisms of action and related infective risk of drugs used for the treatment of immune-mediated and oncologic skin conditions during the daily clinical practice. In general immunosuppressant and antineoplastic agents for dermatologic treatments do not require suspension and do not require special measures, if not those commonly observed. In the case of a COVID19 patient with complication (such as pneumonia, respiratory failure), treatment suspension should always be considered after taking into account the general condition of the patient, the risk-benefit ratio and the pathophysiology of COVID19 infection. The COVID19 emergency pandemic does not imply an under-treatment of existing skin conditions, which together with the SARS-Cov2 infection may jeopardize the patient's life.

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Pulmonary complications of immune checkpoint inhibitors in patients with nonsmall cell lung cancer

Cited by 79 publications

References 152 publications

Pulmonary toxicity of systemic lung cancer therapy

Pulmonary toxicity of systemic lung cancer therapy

Immunotherapy of solid tumors: how safely treat the patients

Systemic immunobiological, immunosuppressant, and oncologic agents for the treatment of dermatologic diseases during theSARS‐CoV‐2 (COVID‐19) pandemic emergency: A quick review for a quick consultation

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