Patient Details Name : RAMA SUBBAMMA C Sex / Age Ref By : Dr. A.V.S. SURESH : Female / 53 Years Case ID : 31206300275 Test Name : Oncocept-Solid Bill. Loc. : Molecular Oncology TS Sample Type : Sample Details Registration Date & Time : 2023-12-11 07:26:32 PM FFPE Block ID- HP3896/23 Report Date & Time : 2023-12-22 06:50:15 PM Clinical History Provided Diagnosis: Metastatic adenocarcinoma of lung Tumor percentage: 65% 31206300275-Mrs. RAMA SUBBAMMA C-53 Years-Female Test Results and Interpretation Positive for ALK gene rearrangement. DNA: No pathogenic variant identified in EGFR, ERBB2, KRAS and BRAF genes. RNA: No fusion identified in ROS1, RET, MET and NTRK genes. Variant Details Fusion Gene Tier EML4::ALK Sensitivity 1A Supporting Reads: 232 In Disease of Interest In Other Diseases In Disease of Interest and Other Diseases UF Unfavorable F Favorable NA Not Available Description ALK, a receptor tyrosine kinase, is recurrently altered by chromosomal rearrangements in various cancer types including anaplastic large cell lymphoma, non-small cell lung cancer and inflammatory myofibroblastic tumors. The EML4-ALK fusion is known to be oncogenic. Crizotinib, ceritinib, alectinib, brigatinib and lorlatinib are FDA-approved for the treatment of patients with ALK-positive lung cancer. In this patient, EML4-ALK fusion variant V1 was noted Eight EML4-ALK variants are generally recognized with a number (1, 2, 3a/b, 4′, 5a/b, 5′, 7, 8) with EML4-ALK variants 1 and 3 being the two most common variants accounting for 75–80 % of the total EML4-ALK variants. Clinical Drug efficacy is considered according to the underlying EML4-ALK variants (v1 -v8) or “short” (v3 and v5) and “long” (v1, v2, v5′, v7, and v8) EML4-ALK variants. Page 1 of 4 Case ID : - 31206300275 Patient Name : RAMA Approved by Dr. Kunjal Patel Page Number : 1 out of 4 Neuberg Center for Genomic Medicine (A Unit Of NSRL) GTPL House Lane, Near East Ebony, Sindhu Bhavan Road, Bodakdev, Ahmedabad | Email: contact@ncgmglobal.com | www.ncgmglobal.com | Phone: 07961618111 / 6357244307 31206300275-Mrs. RAMA SUBBAMMA C-53 Years-Female Variant Details 2-year PFSR was 69.0% (95% CI 49.9–95.4) in group variants 1/2/others versus 32.7% (95% CI 15.6–68.4) in group variants 3a/b for all ALK inhibitors: crizotinib, alectinib, and ceritinib. (Woo CG et al. 2017) References: 1. Zhang SS et al. Lung Cancer. 2021. 2. Lei YY et al. Lung Cancer 2016 3. Christopoulos P et al. International Journal of Cancer. 2018 4. Woo CG et al. Annals of oncology. 2017 Technical Notes AMP/ASCO/CAP Classification Biomarkers that predict response or resistance to US FDA-approved therapies for a specific 1A type of tumor or have been included in professional guidelines as therapeutic, diagnostic, and/or prognostic biomarkers for specific types of tumors. Tier I: Variants of Strong Clinical Significance Biomarkers that predict response or resistance to a therapy based on well-powered 1B studies with consensus from experts in the field, or have diagnostic and/or prognostic significance of certain diseases based on well- powered studies with expert consensus. Biomarkers that predict response or resistance to therapies approved by FDA or 2C Tier II: Variants of Potential Clinical Significance professional societies for a different tumor type (ie, off-label use of a drug), serve as inclusion criteria for clinical trials, or have diagnostic and/or prognostic significance based on the results of multiple small studies; Biomarkers that show plausible therapeutic significance based on preclinical studies, or 2D may assist disease diagnosis and/or prognosis themselves or along with other biomarkers based on small studies or multiple case reports with no consensus Page 2 of 4 Case ID : - 31206300275 Patient Name : RAMA Approved by Dr. Kunjal Patel Page Number : 2 out of 4 Neuberg Center for Genomic Medicine (A Unit Of NSRL) GTPL House Lane, Near East Ebony, Sindhu Bhavan Road, Bodakdev, Ahmedabad | Email: contact@ncgmglobal.com | www.ncgmglobal.com | Phone: 07961618111 / 6357244307 31206300275-Mrs. RAMA SUBBAMMA C-53 Years-Female Technical Notes Not observed at a significant allele frequency in the general or specific subpopulation Tier III: Variants of Unknown Clinical Significance databases, or pan-cancer or tumor-specific variant databases. No convincing published evidence of cancer association Tier IV: Benign or Likely Benign Variants Observed at significant allele frequency in the general or specific subpopulation databases Methodology : Massively Parallel Sequencing (Next Generation Sequencing). Tumor Nucleic acid from the submitted specimen was enriched for the coding regions of genes in the panel and splice site junctions of genes. Paired End Sequencing was performed on Illumina platform (NovaSeq 6000/NextSeq2000). Oncocept solid Panel enables the detection of variants in 52 key solid tumor genes. These genes are well characterized in the published literature and associated with oncology drugs that are FDA approved, part of National Comprehensive Cancer Network (NCCN) guidelines, or in clinical trials. The assay allows concurrent analysis of DNA and RNA. Assay detect multiple types of variants, including hotspots, single nucleotide variants (SNVs), indels, CNVs, and gene fusions, in a single workflow. Genes and Fusion drivers covered in the Panel Oncocept Solid - 52 gene panel AKT1 FGFR3 MET MYC ALK GNA11 MTOR MYCN AR GNAQ NRAS ABL1 BRAF HRAS PDGFRA AKT3 CDK4 IDH1 PIK3CA AXL CTNNB1 IDH2 RAF1 ERG DDR2 JAK1 RET ETV1 EGFR JAK2 ROS1 ETV4 ERBB2 JAK3 SMO ETV5 ERBB3 KIT CCND1 NTRK1 ERBB4 KRAS CDK6 NTKR2 ESR1 MAP2K1 FGFR1 NTKR3 FGFR2 MAP2K2 FGFR4 PPARG Test Limitations Testing has been performed assuming that the sample received belongs to the above named individual(s) and any stated relationships between individuals are accepted as true. Negative (wild type) result does not rule out the presence of a mutation that may be present but below the limits of detection of this assay. The analytical sensitivity of this assay is 5%. Sequencing is performed at a depth of 500x This test does not differentiate between somatic and germline alterations. Additional testing may be necessary to clarify the significance of results if there is a potential hereditary risk. Due to inherent technology limitations, coverage is not uniform across all regions. Hence pathogenic variants present in areas of insufficient coverage may not be analyzed/ reported. The classification and interpretation of all the variants in this assay reflects the current state of scientific understanding at the time this report was issued. In some instances, the classification and interpretation of such variants may change as new scientific information comes to light. Test results should be interpreted in context of clinical findings, tumor sampling, histopathology, and other laboratory data. If results obtained do not match other clinical laboratory findings, please contact the laboratory for possible. Misinterpretation of results may occur if the information provided is inaccurate or incomplete. Page 3 of 4 Case ID : - 31206300275 Patient Name : RAMA Approved by Dr. Kunjal Patel Page Number : 3 out of 4 Neuberg Center for Genomic Medicine (A Unit Of NSRL) GTPL House Lane, Near East Ebony, Sindhu Bhavan Road, Bodakdev, Ahmedabad | Email: contact@ncgmglobal.com | www.ncgmglobal.com | Phone: 07961618111 / 6357244307 Reviewed By Dr. Anjali Deshmukh MBBS, DNB (Path.), PDF Consultant- Molecular Pathologist 31206300275-Mrs. RAMA SUBBAMMA C-53 Years-Female Dr. Kunjal Patel MBBS, DNB, PDF (TMC) Molecular Oncopathologist Page 4 of 4 Case ID : - 31206300275 Patient Name : RAMA Approved by Dr. Kunjal Patel Page Number : 4 out of 4 Neuberg Center for Genomic Medicine (A Unit Of NSRL) GTPL House Lane, Near East Ebony, Sindhu Bhavan Road, Bodakdev, Ahmedabad | Email: contact@ncgmglobal.com | www.ncgmglobal.com | Phone: 07961618111 / 6357244307
