Chemistry-First Approach for Nomination of Personalized Treatment in Lung Cancer

McMillan Elizabeth A.; Ryu Myung-Jeom; Diep Caroline H.; Mendiratta Saurabh; Clemenceau Jean R.; Vaden Rachel M.; Kim Ju-Hwa; Motoyaji Takashi; Covington Kyle R.; Peyton Michael; Huffman Kenneth; Wu Xiaofeng; Girard Luc; Sung Yeojin; Chen Pei-Hsaun; Mallipeddi Prema L.; Lee Joo Young; Hanson Jordan; Voruganti Sukesh; Yu Yunku; Park Sunho; Sudderth Jessica; DeSevo Christopher; Muzny Donna M.; Doddapaneni HarshaVardhan; Gazdar Adi; Gibbs Richard A.; Hwang Tae-Hyun; Heymach John V.; Wistuba Ignacio; Coombes Kevin R.; Williams Noelle S.; Wheeler David A.; MacMillan John B.; Deberardinis Ralph J.; Roth Michael G.; Posner Bruce A.; Minna John D.; Kim Hyun Seok; White Michael A.

首页> 外文期刊>Cell >Chemistry-First Approach for Nomination of Personalized Treatment in Lung Cancer

【24h】

Chemistry-First Approach for Nomination of Personalized Treatment in Lung Cancer

机译：化学 - 提名肺癌个性化治疗的第一方法

获取原文

获取原文并翻译 | 示例

掌桥外文数据库（机构版） >>

开具论文收录证明 >>

文献代查 >>

页面导航

摘要
著录项
相似文献
相关主题

摘要

Diversity in the genetic lesions that cause cancer is extreme. In consequence, a pressing challenge is the development of drugs that target patient-specific disease mechanisms. To address this challenge, we employed a chemistry-first discovery paradigm for de novo identification of druggable targets linked to robust patient selection hypotheses. In particular, a 200,000 compound diversity-oriented chemical library was profiled across a heavily annotated test-bed of 100 cellular models representative of the diverse and characteristic somatic lesions for lung cancer. This approach led to the delineation of 171 chemical-genetic associations, shedding light on the targetability of mechanistic vulnerabilities corresponding to a range of oncogenotypes present in patient populations lacking effective therapy. Chemically addressable addictions to ciliogenesis in TTC21B mutants and GLUT8-dependent serine biosynthesis in KRAS/KEAP1 double mutants are prominent examples. These observations indicate a wealth of actionable opportunities within the complex molecular etiology of cancer.

机译：导致癌症的遗传病变中的多样性是极端的。因此，压迫挑战是靶向患者特异性疾病机制的药物的发展。为了解决这一挑战，我们雇用了化学 - 首先发现范例，用于脱诺鉴定与强大的患者选择假设相关的可药剂目标。特别是，在一个重链的试验床上突出了200,000个化合物的分集化的化学文库，其＆ 100个细胞模型，代表肺癌的多样化和特征体细胞病变。这种方法导致了171个化学遗传关联的划分，揭示了对应于患者患者缺乏有效治疗的患者群体的一系列血晶型的机械脆弱性的靶向。在KRAS / KEAP1双突变体中TTC21B突变体和Glut8依赖性丝状生物合成的化学可寻性上瘾是突出的例子。这些观察结果在癌症的复杂分子病因内表明了丰富的可操作机会。

著录项

来源
《Cell》 |2018年第4期|共44页
作者
McMillan Elizabeth A.; Ryu Myung-Jeom; Diep Caroline H.; Mendiratta Saurabh; Clemenceau Jean R.; Vaden Rachel M.; Kim Ju-Hwa; Motoyaji Takashi; Covington Kyle R.; Peyton Michael; Huffman Kenneth; Wu Xiaofeng; Girard Luc; Sung Yeojin; Chen Pei-Hsaun; Mallipeddi Prema L.; Lee Joo Young; Hanson Jordan; Voruganti Sukesh; Yu Yunku; Park Sunho; Sudderth Jessica; DeSevo Christopher; Muzny Donna M.; Doddapaneni HarshaVardhan; Gazdar Adi; Gibbs Richard A.; Hwang Tae-Hyun; Heymach John V.; Wistuba Ignacio; Coombes Kevin R.; Williams Noelle S.; Wheeler David A.; MacMillan John B.; Deberardinis Ralph J.; Roth Michael G.; Posner Bruce A.; Minna John D.; Kim Hyun Seok; White Michael A.;
展开▼
作者单位

Univ Texas Southwestern Med Ctr Dallas Dept Cell Biol Dallas TX 75390 USA;

Yonsei Univ Coll Med Brain Korea PLUS Project Med Sci 21 Severance Biomed Sci Inst Seoul South Korea;

Univ Texas Southwestern Med Ctr Dallas Dept Cell Biol Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Cell Biol Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Cell Biol Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Cell Biol Dallas TX 75390 USA;

Yonsei Univ Coll Med Brain Korea PLUS Project Med Sci 21 Severance Biomed Sci Inst Seoul South Korea;

Takeda Pharmaceut Co Ltd Pharmaceut Res Div Biomol Res Labs Fujisawa Kanagawa Japan;

Baylor Coll Med Dept Mol &

Human Genet Houston TX 77030 USA;

Univ Texas Southwestern Med Ctr Dallas Hamon Ctr Therapeut Oncol Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Hamon Ctr Therapeut Oncol Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Cell Biol Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Hamon Ctr Therapeut Oncol Dallas TX 75390 USA;

Yonsei Univ Coll Med Brain Korea PLUS Project Med Sci 21 Severance Biomed Sci Inst Seoul South Korea;

Univ Texas Southwestern Med Ctr Dallas Childrens Res Inst Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Biochem Dallas TX 75390 USA;

Yonsei Univ Coll Med Brain Korea PLUS Project Med Sci 21 Severance Biomed Sci Inst Seoul South Korea;

Univ Texas Southwestern Med Ctr Dallas Dept Biochem Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Biochem Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Clin Sci Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Clin Sci Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Childrens Res Inst Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Cell Biol Dallas TX 75390 USA;

Baylor Coll Med Dept Mol &

Human Genet Houston TX 77030 USA;

Baylor Coll Med Dept Mol &

Human Genet Houston TX 77030 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Pathol Dallas TX 75390 USA;

Baylor Coll Med Dept Mol &

Human Genet Houston TX 77030 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Clin Sci Dallas TX 75390 USA;

Univ Texas MD Anderson Canc Ctr Dept Thoracic Head &

Neck Med Oncol Houston TX 77030 USA;

Univ Texas MD Anderson Canc Ctr Translat Mol Pathol Houston TX 77030 USA;

Ohio State Univ Dept Biomed Informat Columbus OH 43210 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Biochem Dallas TX 75390 USA;

Baylor Coll Med Dept Mol &

Human Genet Houston TX 77030 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Biochem Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Childrens Res Inst Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Biochem Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Dept Biochem Dallas TX 75390 USA;

Univ Texas Southwestern Med Ctr Dallas Hamon Ctr Therapeut Oncol Dallas TX 75390 USA;

Yonsei Univ Coll Med Brain Korea PLUS Project Med Sci 21 Severance Biomed Sci Inst Seoul South Korea;

Univ Texas Southwestern Med Ctr Dallas Dept Cell Biol Dallas TX 75390 USA;

展开▼
收录信息
原文格式 PDF
正文语种 eng
中图分类细胞生物学;
关键词

相似文献

外文文献
中文文献
专利

1. Chemistry-First Approach for Nomination of Personalized Treatment in Lung Cancer [J] . McMillan Elizabeth A., Ryu Myung-Jeom, Diep Caroline H., Cell . 2018,第4期

机译：化学 - 提名肺癌个性化治疗的第一方法
2. Chemistry-First Approach for Nomination of Personalized Treatment in Lung Cancer [J] . McMillan Elizabeth A., Ryu Myung-Jeom, Diep Caroline H., Cell . 2018,第4期

机译：化学 - 提名肺癌个性化治疗的第一方法
3. A personalized approach to treatment: use of egfr tyrosine kinase inhibitors for the treatment of non-small-cell lung cancer in Canada [J] . B. Melosky, D. Morris, G. Goss, Current oncology . 2012,第2期

机译：个性化治疗方法：在加拿大使用egfr酪氨酸激酶抑制剂治疗非小细胞肺癌
4. A Sensitive Label-free Quantitation Approach for Personalized Phosphoproteomics Profiling of Non-small Cell Lung Cancer Tissues [C] . Yi-Ting Wang, Chia-Feng Tsai, Pei-Yi Lin, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2012

机译：无小细胞肺癌组织的个性化磷蛋白组学分析的无敏感的定量定量方法
5. The cost effectiveness of screening for early stage lung cancer and the testing and treatment of molecular subgroups among non-small cell lung cancer patients in the province of ontario, canada [D] . Thao, Mallory. 2014

机译：加拿大安大略省非小细胞肺癌患者早期肺癌筛查的成本效益及分子亚群的检测和治疗
6. Chemistry-first approach for nomination of personalized treatment in lung cancer [O] . Elizabeth A. McMillan, Myung-Jeom Ryu, Caroline H. Diep, -1

机译：化学优先提名肺癌个性化治疗的方法
7. Corrigendum: A personalized approach to treatment: use of egfr tyrosine kinase inhibitors for the treatment of non-small-cell lung cancer in Canada [O] . Hirsh, V., Melosky, B., Goss, G., 2012

机译：更正：一种个性化的治疗方法：在加拿大使用egfr酪氨酸激酶抑制剂治疗非小细胞肺癌

Chemistry-First Approach for Nomination of Personalized Treatment in Lung Cancer

摘要

著录项

相似文献

相关主题

期刊订阅