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Literature DB >> 27237027

TPD52L1-ROS1, a new ROS1 fusion variant in lung adenosquamous cell carcinoma identified by comprehensive genomic profiling.

Viola Weijia Zhu¹, Daya Upadhyay², Alexa B Schrock³, Kyle Gowen³, Siraj M Ali³, Sai-Hong Ignatius Ou⁴.

Abstract

Crizotinib was approved for the treatment of ROS1-rearranged non-small cell lung cancer (NSCLC) patients in the US on 11 March, 2016. Interestingly no one companion diagnostic test (CDx) has been approved simultaneously with this approval of crizotinib. Hence, an ideal and adequate CDx will have to be able to identify ROS1 fusions without the knowledge of the fusion partners to ROS1, and as to date there are 13 fusion partners reported for ROS1 in NSCLC. Here we report a novel TPD52L1-ROS1 fusion variant in NSCLC. This novel TPD52L1-ROS1 fusion variant is generated by the fusion of exons 1-3 of TPD52L1 on chromosome 6q22-23 to the exons 33-43 of ROS1 on chromosome 6q22, likely from an intra-chromosomal deletion and subsequent fusion event similar to the generation of EML4-ALK. The predicted TPD52L1-ROS1 protein product contains 655 amino acids comprising of the N-terminal amino acids 1-95 of TPD52L1 and C-terminal amino acids of 1789-2348 of ROS1. In summary, TPD52L1-ROS1 is a novel ROS1 fusion variant in NSCLC identified by comprehensive genomic profiling and should be included in any ROS1 detecting assays that depend on identifying the corresponding fusion partners, such as reverse transcriptase-polymerase chain reaction (RT-PCR).

Entities: Chemical Disease Gene Species

Keywords: Comprehensive genomic profiling; Intra-chromosomal deletion; ROS1-rearranged NSCLC; TPD52L1-ROS1

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Year: 2016 PMID： 27237027 DOI： 10.1016/j.lungcan.2016.04.013

Source DB: PubMed Journal: Lung Cancer ISSN： 0169-5002 Impact factor: 5.705

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Cited

14 in total

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Journal: Oncol Lett Date: 2018-05-22 Impact factor: 2.967

Review 2. Recent Advances in Targeting ROS1 in Lung Cancer.

Authors: Jessica J Lin; Alice T Shaw
Journal: J Thorac Oncol Date: 2017-08-14 Impact factor: 15.609

3. Dual drive coexistence of EML4-ALK and TPM3-ROS1 fusion in advanced lung adenocarcinoma.

Authors: You-Cai Zhu; Xing-Hui Liao; Wen-Xian Wang; Chun-Wei Xu; Wu Zhuang; Jian-Guo Wei; Kai-Qi Du
Journal: Thorac Cancer Date: 2017-12-18 Impact factor: 3.500

4. CEP72-ROS1: A novel ROS1 oncogenic fusion variant in lung adenocarcinoma identified by next-generation sequencing.

Authors: You-Cai Zhu; Yue-Fen Zhou; Wen-Xian Wang; Chun-Wei Xu; Wu Zhuang; Kai-Qi Du; Gang Chen
Journal: Thorac Cancer Date: 2018-03-08 Impact factor: 3.500

5. Prevalence of ROS1 fusion in Chinese patients with non-small cell lung cancer.

Authors: Qing Zhang; Chunyan Wu; Wei Ding; Zhihong Zhang; Xueshan Qiu; Dianbin Mu; Haiqing Zhang; Yanfeng Xi; Jianhua Zhou; Liheng Ma; Shijun Fu; Min Gao; Bo Wang; Juan Deng; Dongmei Lin; Jie Zhang
Journal: Thorac Cancer Date: 2018-11-23 Impact factor: 3.500

6. A novel co-existing ZCCHC8-ROS1 and de-novo MET amplification dual driver in advanced lung adenocarcinoma with a good response to crizotinib.

Authors: You-Cai Zhu; Wen-Xian Wang; Chun-Wei Xu; Wu Zhuang; Zheng-Bo Song; Kai-Qi Du; Gang Chen; Tang-Feng Lv; Yong Song
Journal: Cancer Biol Ther Date: 2018-08-10 Impact factor: 4.742

TPD52L1-ROS1, a new ROS1 fusion variant in lung adenosquamous cell carcinoma identified by comprehensive genomic profiling.

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Review 2. Recent Advances in Targeting ROS1 in Lung Cancer.

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4. CEP72-ROS1: A novel ROS1 oncogenic fusion variant in lung adenocarcinoma identified by next-generation sequencing.

5. Prevalence of ROS1 fusion in Chinese patients with non-small cell lung cancer.

6. A novel co-existing ZCCHC8-ROS1 and de-novo MET amplification dual driver in advanced lung adenocarcinoma with a good response to crizotinib.

7. ROS1 mutation non-small cell lung cancer-access to optimal treatment and outcomes.

8. ROS1 rearrangement and response to crizotinib in Stage IV non-small cell lung cancer.

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