Your search keyword '"Woolston, Annemarie"' showing total 4 results

1. The T cell differentiation landscape is shaped by tumour mutations in lung cancer

Author

Ghorani, Ehsan, Reading, James L, Henry, Jake Y, de Massy, Marc Robert, Rosenthal, Rachel, Turati, Virginia, Joshi, Kroopa, Furness, Andrew J S, Aissa, Assma Ben, Saini, Sunil Kumar, Ramskov, Sofie, Georgiou, Andrew, Sunderland, Mariana Werner, Wong, Yien Ning Sophia, De Mucha, Maria Vila, Day, William, Galvez-Cancino, Felipe, Becker, Pablo D, Uddin, Imran, Ismail, Mazlina, Ronel, Tahel, Woolston, Annemarie, Jamal-Hanjani, Mariam, Veeriah, Selvaraju, Birkbak, Nicolai J., Wilson, Gareth A, Litchfield, Kevin, Conde, Lucia, Guerra-Assunção, José Afonso, Blighe, Kevin, Biswas, Dhruva, Salgado, Roberto, Lund, Tom, Al Bakir, Maise, Moore, David A, Hiley, Crispin T, Loi, Sherene, Sun, Yuxin, Yuan, Yinyin, AbdulJabbar, Khalid, Turajilic, Samra, Herrero, Javier, Enver, Tariq, Hadrup, Sine R., Hackshaw, Allan, Peggs, Karl S, McGranahan, Nicholas, Chain, Benny, Swanton, Charles, Quezada, Sergio A, Ghorani, Ehsan, Reading, James L, Henry, Jake Y, de Massy, Marc Robert, Rosenthal, Rachel, Turati, Virginia, Joshi, Kroopa, Furness, Andrew J S, Aissa, Assma Ben, Saini, Sunil Kumar, Ramskov, Sofie, Georgiou, Andrew, Sunderland, Mariana Werner, Wong, Yien Ning Sophia, De Mucha, Maria Vila, Day, William, Galvez-Cancino, Felipe, Becker, Pablo D, Uddin, Imran, Ismail, Mazlina, Ronel, Tahel, Woolston, Annemarie, Jamal-Hanjani, Mariam, Veeriah, Selvaraju, Birkbak, Nicolai J., Wilson, Gareth A, Litchfield, Kevin, Conde, Lucia, Guerra-Assunção, José Afonso, Blighe, Kevin, Biswas, Dhruva, Salgado, Roberto, Lund, Tom, Al Bakir, Maise, Moore, David A, Hiley, Crispin T, Loi, Sherene, Sun, Yuxin, Yuan, Yinyin, AbdulJabbar, Khalid, Turajilic, Samra, Herrero, Javier, Enver, Tariq, Hadrup, Sine R., Hackshaw, Allan, Peggs, Karl S, McGranahan, Nicholas, Chain, Benny, Swanton, Charles, and Quezada, Sergio A

Abstract

Tumour mutational burden (TMB) predicts immunotherapy outcome in non-small cell lung cancer (NSCLC), consistent with immune recognition of tumour neoantigens. However, persistent antigen exposure is detrimental for T cell function. How TMB affects CD4 and CD8 T cell differentiation in untreated tumours, and whether this affects patient outcomes is unknown. Here we paired high-dimensional flow cytometry, exome, single-cell and bulk RNA sequencing from patients with resected, untreated NSCLC to examine these relationships. TMB was associated with compartment-wide T cell differentiation skewing, characterized by loss of TCF7-expressing progenitor-like CD4 T cells, and an increased abundance of dysfunctional CD8 and CD4 T cell subsets, with significant phenotypic and transcriptional similarity to neoantigen-reactive CD8 T cells. A gene signature of redistribution from progenitor-like to dysfunctional states associated with poor survival in lung and other cancer cohorts. Single-cell characterization of these populations informs potential strategies for therapeutic manipulation in NSCLC.

Published

2020

2. Genetic loci associated with an earlier age at onset in multiplex schizophrenia.

Author

Woolston, Annemarie L, Woolston, Annemarie L, Hsiao, Po-Chang, Kuo, Po-Hsiu, Wang, Shi-Heng, Lien, Yin-Ju, Liu, Chih-Min, Hwu, Hai-Gwo, Lu, Tzu-Pin, Chuang, Eric Y, Chang, Li-Ching, Chen, Chien-Hsiun, Wu, Jer-Yuarn, Tsuang, Ming T, Chen, Wei J, Woolston, Annemarie L, Woolston, Annemarie L, Hsiao, Po-Chang, Kuo, Po-Hsiu, Wang, Shi-Heng, Lien, Yin-Ju, Liu, Chih-Min, Hwu, Hai-Gwo, Lu, Tzu-Pin, Chuang, Eric Y, Chang, Li-Ching, Chen, Chien-Hsiun, Wu, Jer-Yuarn, Tsuang, Ming T, and Chen, Wei J

Abstract

An earlier age at onset (AAO) has been associated with greater genetic loadings in schizophrenia. This study aimed to identify modifier loci associated with an earlier AAO of schizophrenia. A genome-wide association analysis (GWAS) was conducted in 94 schizophrenia probands with the earliest AAO and 91 with the latest AAO. Candidate single nucleotide polymorphisms (SNPs) were then genotyped in the co-affected siblings and unrelated probands. Multi-SNP genetic risk scores (GRS) composed of the candidate loci were used to distinguish patients with an early or late AAO. The 14-SNP GRS could distinguish the co-affected siblings (n = 90) of the earliest probands from those (n = 91) of the latest probands. When 132 patients with an earlier AAO and 158 patients with a later AAO were included, a significant trend in the 14-SNP GRS was detected among those unrelated probands from 4 family groups with the earliest, earlier, later, and latest AAO. The overall effect of the 14 SNPs on an AAO in schizophrenia was verified using co-affected siblings of the GWAS probands and trend effect across unrelated patients. Preliminary network analysis of these loci revealed the involvement of PARK2, a gene intensively reported in Parkinson's disease and schizophrenia research.

Published

2017

3. Genetic loci associated with an earlier age at onset in multiplex schizophrenia.

Author

Woolston, Annemarie L, Woolston, Annemarie L, Hsiao, Po-Chang, Kuo, Po-Hsiu, Wang, Shi-Heng, Lien, Yin-Ju, Liu, Chih-Min, Hwu, Hai-Gwo, Lu, Tzu-Pin, Chuang, Eric Y, Chang, Li-Ching, Chen, Chien-Hsiun, Wu, Jer-Yuarn, Tsuang, Ming T, Chen, Wei J, Woolston, Annemarie L, Woolston, Annemarie L, Hsiao, Po-Chang, Kuo, Po-Hsiu, Wang, Shi-Heng, Lien, Yin-Ju, Liu, Chih-Min, Hwu, Hai-Gwo, Lu, Tzu-Pin, Chuang, Eric Y, Chang, Li-Ching, Chen, Chien-Hsiun, Wu, Jer-Yuarn, Tsuang, Ming T, and Chen, Wei J

Abstract

An earlier age at onset (AAO) has been associated with greater genetic loadings in schizophrenia. This study aimed to identify modifier loci associated with an earlier AAO of schizophrenia. A genome-wide association analysis (GWAS) was conducted in 94 schizophrenia probands with the earliest AAO and 91 with the latest AAO. Candidate single nucleotide polymorphisms (SNPs) were then genotyped in the co-affected siblings and unrelated probands. Multi-SNP genetic risk scores (GRS) composed of the candidate loci were used to distinguish patients with an early or late AAO. The 14-SNP GRS could distinguish the co-affected siblings (n = 90) of the earliest probands from those (n = 91) of the latest probands. When 132 patients with an earlier AAO and 158 patients with a later AAO were included, a significant trend in the 14-SNP GRS was detected among those unrelated probands from 4 family groups with the earliest, earlier, later, and latest AAO. The overall effect of the 14 SNPs on an AAO in schizophrenia was verified using co-affected siblings of the GWAS probands and trend effect across unrelated patients. Preliminary network analysis of these loci revealed the involvement of PARK2, a gene intensively reported in Parkinson's disease and schizophrenia research.

Published

2017

4. Spatial heterogeneity of the T cell receptor repertoire reflects the mutational landscape in lung cancer

Author

Joshi, Kroopa, Robert de Massy, Marc, Ismail, Mazlina, Reading, James L., Uddin, Imran, Woolston, Annemarie, Hatipoglu, Emine, Oakes, Theres, Rosenthal, Rachel, Peacock, Thomas, Ronel, Tahel, Noursadeghi, Mahdad, Turati, Virginia, Georgiou, Andrew, Furness, Andrew J. S., Wong, Yien Ning Sophia, Ben Aissa, Assma, Werner Sunderland, Mariana, Jamal-Hanjani, Mariam, Veeriah, Selvaraju, Birkbak, Nicolai Juul, Wilson, Gareth A., Hiley, Crispin T, Ghorani, Ehsan, Guerra-Assunção, José Afonso, Herrero, Javier, Enver, Tariq, Hadrup, Sine R., Hackshaw, Allan, Peggs, Karl S, McGranahan, Nicholas, Swanton, Charles, Quezada, Sergio A., Chain, Benny, Joshi, Kroopa, Robert de Massy, Marc, Ismail, Mazlina, Reading, James L., Uddin, Imran, Woolston, Annemarie, Hatipoglu, Emine, Oakes, Theres, Rosenthal, Rachel, Peacock, Thomas, Ronel, Tahel, Noursadeghi, Mahdad, Turati, Virginia, Georgiou, Andrew, Furness, Andrew J. S., Wong, Yien Ning Sophia, Ben Aissa, Assma, Werner Sunderland, Mariana, Jamal-Hanjani, Mariam, Veeriah, Selvaraju, Birkbak, Nicolai Juul, Wilson, Gareth A., Hiley, Crispin T, Ghorani, Ehsan, Guerra-Assunção, José Afonso, Herrero, Javier, Enver, Tariq, Hadrup, Sine R., Hackshaw, Allan, Peggs, Karl S, McGranahan, Nicholas, Swanton, Charles, Quezada, Sergio A., and Chain, Benny

Abstract

Somatic mutations together with immunoediting drive extensive heterogeneity within non-small-cell lung cancer (NSCLC). Herein we examine heterogeneity of the T cell antigen receptor (TCR) repertoire. The number of TCR sequences selectively expanded in tumors varies within and between tumors and correlates with the number of nonsynonymous mutations. Expanded TCRs can be subdivided into TCRs found in all tumor regions (ubiquitous) and those present in a subset of regions (regional). The number of ubiquitous and regional TCRs correlates with the number of ubiquitous and regional nonsynonymous mutations, respectively. Expanded TCRs form part of clusters of TCRs of similar sequence, suggestive of a spatially constrained antigen-driven process. CD8+ tumor-infiltrating lymphocytes harboring ubiquitous TCRs display a dysfunctional tissue-resident phenotype. Ubiquitous TCRs are preferentially detected in the blood at the time of tumor resection as compared to routine follow-up. These findings highlight a noninvasive method to identify and track relevant tumor-reactive TCRs for use in adoptive T cell immunotherapy.

Published

2019