A Prospective PCR-Based Screening for the <i>EML4-ALK</i> Oncogene in Non–Small Cell Lung Cancer

Soda, Manabu; Isobe, Kazutoshi; Inoue, Akira; Maemondo, Makoto; Oizumi, Satoshi; Fujita, Yuka; Gemma, Akihiko; Yamashita, Yuichi; Ueno, Toshihide; Takeuchi, Kengo; Choi, Young Lim; Miyazawa, Hitoshi; Tanaka, Tomoaki; Hagiwara, Koichi; Mano, Hiroyuki

doi:10.1158/1078-0432.ccr-11-2947

Cited by 113 publications

(108 citation statements)

References 29 publications

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“…Cytological lung carcinoma specimens frozen at -80°C were informative for fusion between the echinoderm microtubule-associated protein-like 4 (EML4) and the anaplastic lymphoma kinase (ALK) genes [67]. Specimens were mixed with a buffer preventing RNA degradation before freezing in the latter study.…”

Section: Other Ancillary Testingmentioning

confidence: 99%

Pre-analytical issues in effusion cytology

Michael

Davidson²

2016

Pleura and Peritoneum

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Effusions or body cavity fluids are amongst the most commonly submitted samples to the cytology laboratory. Knowledge of proper collection, storage, preservation and processing techniques is essential to ensure proper handling and successful analysis of the sample. This article describes how the effusions should be collected and proper conditions for submission. The different processing techniques to extract the cellular material and prepare slides satisfactory for microscopic evaluation are described such as direct smears, cytospins, liquid based preparations and cell blocks. The article further elaborates on handling the specimens for additional ancillary testing such as immunostaining and molecular tests, including predictive ones, as well as future research approaches.

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Section: Other Ancillary Testingmentioning

confidence: 99%

Pre-analytical issues in effusion cytology

Michael

Davidson²

2016

Pleura and Peritoneum

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“…156,166 Although at the time of writing RT-PCR and NGS are not approved by FDA in the United States as first-line methods for determining ALK status in selection of patients for ALK inhibitor therapy, these approaches have shown comparable performance with IHC 163e165 when designed to detect the majority of fusions, and are standard practice in many other countries. 163e165,167 These methods are highly specific for most fusions, 97,168,169 and patients with positive results should be treated with an ALK inhibitor, although patients with negative results may benefit from a more sensitive method to exclude the possibility of a variant fusion. Similarly, amplicon-based NGS assays of DNA may likewise fail to detect all fusion variants, and therefore a capture-based DNA or RNA approach is preferred for NGS testing for ALK fusions.…”

Section: Recommendationmentioning

confidence: 99%

Analytical Validation of BRAF Mutation Testing from Circulating Free DNA Using the Amplification Refractory Mutation Testing System

Aung

Donald

Ellison

et al. 2014

The Journal of Molecular Diagnostics

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Context: In 2013, an evidence-based guideline was published by the College of American Pathologists, the International Association for the Study of Lung Cancer, and the Association for Molecular Pathology to set standards for the molecular analysis of lung cancers to guide treatment decisions with targeted inhibitors. New evidence has prompted an evaluation of additional laboratory technologies, targetable genes, patient populations, and tumor types for testing. Objective: To systematically review and update the 2013 guideline to affirm its validity; to assess the evidence of new genetic discoveries, technologies, and therapies; and to issue an evidence-based update. Design: The College of American Pathologists, the International Association for the Study of Lung Cancer, and the Association for Molecular Pathology convened an expert panel to develop an evidence-based guideline to help define the key questions and literature search terms, review abstracts and full articles, and draft recommendations. Results: Eighteen new recommendations were drafted. The panel also updated 3 recommendations from the 2013 guideline. Conclusions: The 2013 guideline was largely reaffirmed with updated recommendations to allow testing of cytology samples, require improved assay sensitivity, and recommend against the use of

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“…This fusion results from the rearrangement within chromosome 2 [inv (2)(p21p23)] and fusion of the 5' portion of EML4 with the 3' portion of ALK (6). At least 14 variants of the EML4-ALK fusion gene have been reported thus far, encoding for the cytoplasmic portion of ALK protein and containing varying lengths of EML4 (19). Variants v1, v2, v3a and v3b of EML4-ALK fusion gene are the most commonly detected, together accounting for more than 90% of variants in some series (20).…”

Section: Molecular Pathology Of Alk-rearranged Nsclcmentioning

confidence: 99%

“…Most of the current guidelines do not include it ALK RT-PCR in their diagnostic algorithms, as the rate of failures and falsenegative tests can be significant. Nevertheless, RT-PCR can find its best utility in samples not suitable for tissue blocking, mainly represented by bronchial washing fluid and pleural effusions (19,58). RT-PCR could represent a useful tool to detect fusion variants of the EML4-ALK fusion gene which otherwise, besides harboring unclear clinical significance (see above), can be currently revealed by nextgeneration genomic and transcriptomic analyses (see next paragraph).…”

Section: Reverse Transcriptase-polymerase Chain Reaction (Rt-pcr)mentioning

confidence: 99%

Tackling ALK in non-small cell lung cancer: the role of novel inhibitors

Facchinetti¹,

Tiseo²,

Maïo³

et al. 2016

Transl. Lung Cancer Res.

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Abstract:Crizotinib is an oral inhibitor of anaplastic lymphoma kinase (ALK) with remarkable clinical activity in patients suffering from ALK-rearranged non-small cell lung cancer (NSCLC), accounting to its superiority compared to chemotherapy. Unfortunately, virtually all ALK-rearranged tumors acquire resistance to crizotinib, frequently within one year since the treatment initiation. To date, therapeutic strategies to overcome crizotinib resistance have focused on the use of more potent and structurally different compounds. Second-generation ALK inhibitors such as ceritinib (LDK378), alectinib (CH5424802/ RO5424802) and brigatinib (AP26113) have shown relevant clinical activity, consequently fostering their rapid clinical development and their approval by health agencies. The third-generation inhibitor lorlatinib (PF-06463922), selectively active against ALK and ROS1, harbors impressive biological potency; its efficacy in reversing resistance to crizotinib and to other ALK inhibitors is being proven by early clinical trials. The NTRK1-3 and ROS1 inhibitor entrectinib (RXDX-101) has been reported to act against NSCLC harboring ALK fusion proteins too. Despite the quick development of these novel agents, several issues remain to be discussed in the treatment of patients suffering from ALK-rearranged NSCLC. This position paper will discuss the development, the current evidence and approvals, as long as the future perspectives of new ALK inhibitors beyond crizotinib. Clinical behaviors of ALK-rearranged NSCLC vary significantly among patients and differential molecular events responsible of crizotinib resistance account for the most important quote of this heterogeneity. The precious availability of a wide range of active anti-ALK compounds should be approached in a critical and careful perspective, in order to develop treatment strategies tailored on the disease evolution of every single patient.

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A Prospective PCR-Based Screening for the EML4-ALK Oncogene in Non–Small Cell Lung Cancer

Cited by 113 publications

References 29 publications

Pre-analytical issues in effusion cytology

Pre-analytical issues in effusion cytology

Analytical Validation of BRAF Mutation Testing from Circulating Free DNA Using the Amplification Refractory Mutation Testing System

Tackling ALK in non-small cell lung cancer: the role of novel inhibitors

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