Next-Generation Sequencing Approach to Non–Small Cell Lung Carcinoma Yields More Actionable Alterations

Mehrad, Mitra; Bittar, Humberto E. Trejo; Đačić, Sanja

doi:10.5858/arpa.2017-0046-oa

Cited by 25 publications

(14 citation statements)

References 28 publications

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“…Akciğer adenokarsinomlarının yaklaşık %1-2'sinde görülür ve yine aynı ALK gibi ROS1 rearranjmanı saptanan hastalar bir tirozin kinaz inhibitörü olan krizotinibe yanıt verir (12,19). ROS1 rearranjmanı gösterebilmek için FİSH, PCR, yeni nesil sekanslama gibi pek çok yöntem kullanılabilir (20,21). ROS1'de uygulanan FİSH yöntemi ALK rearranjmanı için uygulanan yöntemle aynı olup, pozitiflik sınır değeri de %15 ve üstü olarak belirlenmiştir.…”

Section: Ros1 Rearranjmanıunclassified

Molecular Pathology of Lung Cancer

Bozkurtlar¹,

Kaya²

2018

Nts

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Section: Ros1 Rearranjmanıunclassified

Molecular Pathology of Lung Cancer

Bozkurtlar¹,

Kaya²

2018

Nts

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“…The National Comprehensive Cancer Network Guidelines recommends testing a panel of genes for NSCLC, which consists of epidermal growth factor ( EGFR ) mutations, anapestic lymphoma kinase ( ALK ) rearrangements, and c-ros oncogene 1 ( ROS1 ) rearrangements. These biomarkers are considered the “must-tests” biomarkers in lung cancer patient diagnosis and are analyzed by single-gene assays such as PCR, immunohistochemistry (IHC), and FISH [ 20 , 55 , 56 , 57 , 58 , 59 , 60 ]. Sanger sequencing, qPCR, ddPCR, IHC, and FISH are regarded as the gold standard techniques of molecular analysis in clinical practice, while tumor-only sequencing, matched-tumor, and normal-tissue sequencing are the gold standards in somatic mutation detection [ 18 , 61 ].…”

Section: Advancement Of Molecular Strategies and Techniques Used Tmentioning

confidence: 99%

Genetic Markers in Lung Cancer Diagnosis: A Review

Wadowska

Bil‐Lula

Trembecki

et al. 2020

IJMS

146

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Lung cancer is the most often diagnosed cancer in the world and the most frequent cause of cancer death. The prognosis for lung cancer is relatively poor and 75% of patients are diagnosed at its advanced stage. The currently used diagnostic tools are not sensitive enough and do not enable diagnosis at the early stage of the disease. Therefore, searching for new methods of early and accurate diagnosis of lung cancer is crucial for its effective treatment. Lung cancer is the result of multistage carcinogenesis with gradually increasing genetic and epigenetic changes. Screening for the characteristic genetic markers could enable the diagnosis of lung cancer at its early stage. The aim of this review was the summarization of both the preclinical and clinical approaches in the genetic diagnostics of lung cancer. The advancement of molecular strategies and analytic platforms makes it possible to analyze the genome changes leading to cancer development—i.e., the potential biomarkers of lung cancer. In the reviewed studies, the diagnostic values of microsatellite changes, DNA hypermethylation, and p53 and KRAS gene mutations, as well as microRNAs expression, have been analyzed as potential genetic markers. It seems that microRNAs and their expression profiles have the greatest diagnostic potential value in lung cancer diagnosis, but their quantification requires standardization.

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“…Genomic Marker Assessment.-The assessment of genomic markers, particularly for mutations and gene rearrangements in tumors, 20,21,39 is evolving quickly, with preparations ranging from DNA isolation 40 and RNA probes 41,42 to next-generation sequencing. 43,44 The amount of sample required varies with the genomic technology. For DNA extraction from CNB histologic preparations, 1 lg of DNA is required.…”

Section: Sample Contains Adequate Materials For Intended Assessmentmentioning

confidence: 99%

Needle Biopsy Adequacy in the Era of Precision Medicine and Value-Based Health Care

Pritzker

Nieminen

2019

Archives of Pathology &Amp; Laboratory Medicine

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Context.— Needle biopsy of diseased tissue is an essential diagnostic tool that is becoming even more important as precision medicine develops. However, the capability of this modality to efficiently provide samples adequate for diagnostic and prognostic analysis remains quite limited relative to current diagnostic needs. For physicians and patients, inadequate biopsy frequently leads to diagnostic delay, procedure duplication, or insufficient information about tumor biology leading to delay in treatment; for health systems, this results in substantial incremental costs and inefficient use of scarce specialized diagnostic resources. Objective.— To review current needle biopsy technology, devices, and practice with a perspective to identify current limitations and opportunities for improvement in the context of advancing precision medicine. Data Sources.— PubMed searches of fine-needle aspiration and core needle biopsy devices and similar technologies were made generally, by tissue site, and by adequacy as well as by health economics of these technologies. Conclusions.— Needle biopsy adequacy can be improved by recognizing the importance of this diagnostic tool by promoting common criteria for needle biopsy adequacy; by optimizing needle biopsy procedural technique, technologies, clinical practice, professional education, and quality assurance; and by bundling biopsy procedure costs with downstream diagnostic modalities to provide better accountability and incentives to improve the diagnostic process.

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Next-Generation Sequencing Approach to Non–Small Cell Lung Carcinoma Yields More Actionable Alterations

Cited by 25 publications

References 28 publications

Molecular Pathology of Lung Cancer

Molecular Pathology of Lung Cancer

Genetic Markers in Lung Cancer Diagnosis: A Review

Needle Biopsy Adequacy in the Era of Precision Medicine and Value-Based Health Care

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