Your search keyword '"Roychoudhuri, Rahul"' showing total 21 results

1. Intratumoral antigen signaling traps CD8+ T cells to confine exhaustion to the tumor site.

Author

Takahashi, Munetomo, So, Tsz Y., Chamberlain-Evans, Vitalina, Hughes, Robert, Yam-Puc, Juan Carlos, Kania, Katarzyna, Ruhle, Michelle, Mann, Tiffeney, Schuijs, Martijn J., Coupland, Paul, Naisbitt, Dean, Halim, Timotheus Y. F., Lyons, Paul A., Lio, Pietro, Roychoudhuri, Rahul, Okkenhaug, Klaus, Adams, David J., Smith, Ken G. C., Jodrell, Duncan I., and Chapman, Michael A.

Subjects

T-cell exhaustion, REGULATORY T cells, CLONE cells, T cells, ANTIGENS

Abstract

Immunotherapy advances have been hindered by difficulties in tracking the behaviors of lymphocytes after antigen signaling. Here, we assessed the behavior of T cells active within tumors through the development of the antigen receptor signaling reporter (AgRSR) mouse, fate-mapping lymphocytes responding to antigens at specific times and locations. Contrary to reports describing the ready egress of T cells out of the tumor, we find that intratumoral antigen signaling traps CD8+ T cells in the tumor. These clonal populations expand and become increasingly exhausted over time. By contrast, antigen-signaled regulatory T cell (Treg) clonal populations readily recirculate out of the tumor. Consequently, intratumoral antigen signaling acts as a gatekeeper to compartmentalize CD8+ T cell responses, even within the same clonotype, thus enabling exhausted T cells to remain confined to a specific tumor tissue site. Editor's summary: An understanding of how T cells behave after antigen signaling is critical to improving immunotherapies. Takahashi et al. developed the antigen receptor signaling reporter (AgRSR) mice to fate-map T cells responding to antigen signals. In tumors, they showed that antigen engagement caused clonally expanded CD8 T cells to be retained within tumors, resulting in T cell exhaustion. Whereas antigen engagement of regulatory T cells (Tregs) within tumors similarly induced clonal expansion, Tregs were able to recirculate. These results provide insight into T cell behaviors that may limit antitumor responses and introduce a system for tracking adaptive immunity. —Christiana Fogg [ABSTRACT FROM AUTHOR]

Published

2024

2. GS-TCGA: Gene Set-Based Analysis of The Cancer Genome Atlas.

Author

Baird, Tarrion and Roychoudhuri, Rahul

Published

2024

3. Tumour-retained activated CCR7+ dendritic cells are heterogeneous and regulate local anti-tumour cytolytic activity.

Author

Lee, Colin Y. C., Kennedy, Bethany C., Richoz, Nathan, Dean, Isaac, Tuong, Zewen K., Gaspal, Fabrina, Li, Zhi, Willis, Claire, Hasegawa, Tetsuo, Whiteside, Sarah K., Posner, David A., Carlesso, Gianluca, Hammond, Scott A., Dovedi, Simon J., Roychoudhuri, Rahul, Withers, David R., and Clatworthy, Menna R.

Subjects

DENDRITIC cells, CYTOTOXIC T cells, T cells, ANTIGEN presentation, LYMPH nodes, CELL migration

Abstract

Tumour dendritic cells (DCs) internalise antigen and upregulate CCR7, which directs their migration to tumour-draining lymph nodes (dLN). CCR7 expression is coupled to an activation programme enriched in regulatory molecule expression, including PD-L1. However, the spatio-temporal dynamics of CCR7+ DCs in anti-tumour immune responses remain unclear. Here, we use photoconvertible mice to precisely track DC migration. We report that CCR7+ DCs are the dominant DC population that migrate to the dLN, but a subset remains tumour-resident despite CCR7 expression. These tumour-retained CCR7+ DCs are phenotypically and transcriptionally distinct from their dLN counterparts and heterogeneous. Moreover, they progressively downregulate the expression of antigen presentation and pro-inflammatory transcripts with more prolonged tumour dwell-time. Tumour-residing CCR7+ DCs co-localise with PD-1+CD8+ T cells in human and murine solid tumours, and following anti-PD-L1 treatment, upregulate stimulatory molecules including OX40L, thereby augmenting anti-tumour cytolytic activity. Altogether, these data uncover previously unappreciated heterogeneity in CCR7+ DCs that may underpin a variable capacity to support intratumoural cytotoxic T cells. Recognition of tumour antigen induces dendritic cell activation and migration to the lymph node. Here, the authors use photoconvertible mice to demonstrate that some activated dendritic cells are retained in tumours and gradually lose function, but their ability to support local anti-tumour responses can be augmented by anti-PD-L1 blockade. [ABSTRACT FROM AUTHOR]

Published

2024

4. Tumour-retained activated CCR7+ dendritic cells are heterogeneous and regulate local anti-tumour cytolytic activity.

Author

Lee, Colin Y. C., Kennedy, Bethany C., Richoz, Nathan, Dean, Isaac, Tuong, Zewen K., Gaspal, Fabrina, Li, Zhi, Willis, Claire, Hasegawa, Tetsuo, Whiteside, Sarah K., Posner, David A., Carlesso, Gianluca, Hammond, Scott A., Dovedi, Simon J., Roychoudhuri, Rahul, Withers, David R., and Clatworthy, Menna R.

Subjects

DENDRITIC cells, CYTOTOXIC T cells, T cells, ANTIGEN presentation, LYMPH nodes, CELL migration

Abstract

Tumour dendritic cells (DCs) internalise antigen and upregulate CCR7, which directs their migration to tumour-draining lymph nodes (dLN). CCR7 expression is coupled to an activation programme enriched in regulatory molecule expression, including PD-L1. However, the spatio-temporal dynamics of CCR7+ DCs in anti-tumour immune responses remain unclear. Here, we use photoconvertible mice to precisely track DC migration. We report that CCR7+ DCs are the dominant DC population that migrate to the dLN, but a subset remains tumour-resident despite CCR7 expression. These tumour-retained CCR7+ DCs are phenotypically and transcriptionally distinct from their dLN counterparts and heterogeneous. Moreover, they progressively downregulate the expression of antigen presentation and pro-inflammatory transcripts with more prolonged tumour dwell-time. Tumour-residing CCR7+ DCs co-localise with PD-1+CD8+ T cells in human and murine solid tumours, and following anti-PD-L1 treatment, upregulate stimulatory molecules including OX40L, thereby augmenting anti-tumour cytolytic activity. Altogether, these data uncover previously unappreciated heterogeneity in CCR7+ DCs that may underpin a variable capacity to support intratumoural cytotoxic T cells. Recognition of tumour antigen induces dendritic cell activation and migration to the lymph node. Here, the authors use photoconvertible mice to demonstrate that some activated dendritic cells are retained in tumours and gradually lose function, but their ability to support local anti-tumour responses can be augmented by anti-PD-L1 blockade. [ABSTRACT FROM AUTHOR]

Published

2024

5. IL-2 is inactivated by the acidic pH environment of tumors enabling engineering of a pH-selective mutein.

Author

Gaggero, Silvia, Martinez-Fabregas, Jonathan, Cozzani, Adeline, Fyfe, Paul K., Leprohon, Malo, Yang, Jie, Thomasen, F. Emil, Winkelmann, Hauke, Magnez, Romain, Conti, Alberto G., Wilmes, Stephan, Pohler, Elizabeth, van Gijsel Bonnello, Manuel, Thuru, Xavier, Quesnel, Bruno, Soncin, Fabrice, Piehler, Jacob, Lindorff-Larsen, Kresten, Roychoudhuri, Rahul, and Moraga, Ignacio

Subjects

TUMOR microenvironment, IMMUNE response, KILLER cells, T cells, CELL physiology, T cell receptors

Abstract

Cytokines interact with their receptors in the extracellular space to control immune responses. How the physicochemical properties of the extracellular space influence cytokine signaling is incompletely elucidated. Here, we show that the activity of interleukin-2 (IL-2), a cytokine critical to T cell immunity, is profoundly affected by pH, limiting IL-2 signaling within the acidic environment of tumors. Generation of lactic acid by tumors limits STAT5 activation, effector differentiation, and antitumor immunity by CD8+ T cells and renders high-dose IL-2 therapy poorly effective. Directed evolution enabled selection of a pH-selective IL-2 mutein (Switch-2). Switch-2 binds the IL-2 receptor subunit IL-2Rα with higher affinity, triggers STAT5 activation, and drives CD8+ T cell effector function more potently at acidic pH than at neutral pH. Consequently, high-dose Switch-2 therapy induces potent immune activation and tumor rejection with reduced on-target toxicity in normal tissues. Last, we show that sensitivity to pH is a generalizable property of a diverse range of cytokines with broad relevance to immunity and immunotherapy in healthy and diseased tissues. Acid-tolerant IL-2 targets tumors: Hypoxic and acidic conditions prevalent in the tumor microenvironment present a formidable challenge for host lymphocytes trying to eradicate cancer cells. IL-2, a cytokine supporting CD8 T cell and NK cell functions, exhibits markedly compromised binding to the IL-2Rα receptor chain at pH 6 and below. Gaggero et al. used directed evolution to screen for IL-2 variants with mutations at the receptor interface that enhanced receptor binding at low pH. A mutated "Switch-2" variant of IL-2 with strong receptor binding at pH 6 but minimal interaction at neutral pH exhibited enhanced in vivo antitumor activity in mice. Recognition of the pH sensitivity of IL-2 and other cytokines will spur engineering of cytokine variants capable of enhanced performance in the acidic tumor microenvironment. [ABSTRACT FROM AUTHOR]

Published

2022

6. CCR8 marks highly suppressive Treg cells within tumours but is dispensable for their accumulation and suppressive function.

Author

Whiteside, Sarah K., Grant, Francis M., Gyori, David S., Conti, Alberto G., Imianowski, Charlotte J., Kuo, Paula, Nasrallah, Rabab, Sadiyah, Firas, Lira, Sergio A., Tacke, Frank, Eil, Robert L., Burton, Oliver T., Dooley, James, Liston, Adrian, Okkenhaug, Klaus, Yang, Jie, and Roychoudhuri, Rahul

Subjects

REGULATORY T cells, HOMEOSTASIS, LYMPHOID tissue, TUMORS, T cells

Abstract

CD4+ regulatory T (Treg) cells, dependent upon the transcription factor Foxp3, contribute to tumour immunosuppression but are also required for immune homeostasis. There is interest in developing therapies that selectively target the immunosuppressive function of Treg cells within tumours without disrupting their systemic anti‐inflammatory function. High levels of expression of chemokine (C‐C motif) receptor 8 (CCR8) discriminate Treg cells within tumours from those found in systemic lymphoid tissues. It has recently been proposed that disruption of CCR8 function using blocking anti‐CCR8 antibodies results in reduced accumulation of Treg cells within tumours and disruption of their immunosuppressive function. Here, using Ccr8−/− mice, we show that CCR8 function is not required for Treg cell accumulation or immunosuppression in the context of syngeneic MC38 colorectal adenocarcinoma and B16 melanoma tumours. We observed high levels of CCR8 expression on tumour‐infiltrating Treg cells which were abolished in Ccr8−/− mice. High levels of CCR8 marked cells with high levels of suppressive function. However, whereas systemic ablation of Treg cells resulted in strikingly diminished tumour burden, growth of subcutaneously implanted tumours was unaffected by systemic CCR8 loss. Consistently, we observed minimal impact of systemic CCR8 ablation on the frequency, phenotype and function of tumour‐infiltrating Treg cells and conventional T (Tconv) function. These findings suggest that CCR8 is not required for Treg cell accumulation and immunosuppressive function within tumours and that depletion of CCR8+ Treg cells rather than blockade of CCR8 function is a more promising avenue for selective immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2021

7. Regulation of regulatory T cells in cancer.

Author

Stockis, Julie, Roychoudhuri, Rahul, and Halim, Timotheus Y. F.

Subjects

T cells, CANCER cells, PSYCHONEUROIMMUNOLOGY, CELLULAR control mechanisms, CYTOKINE receptors

Abstract

Summary: The inflammatory response to transformed cells forms the cornerstone of natural or therapeutically induced protective immunity to cancer. Regulatory T (Treg) cells are known for their critical role in suppressing inflammation, and therefore can antagonize effective anti‐cancer immune responses. As such, Treg cells can play detrimental roles in tumour progression and in the response to both conventional and immune‐based cancer therapies. Recent advances in our understanding of Treg cells reveal complex niche‐specific regulatory programmes and functions, which are likely to extrapolate to cancer. The regulation of Treg cells is reliant on upstream cues from haematopoietic and non‐immune cells, which dictates their genetic, epigenetic and downstream functional programmes. In this review we will discuss how Treg cells are themselves regulated in normal and transformed tissues, and the implications of this cross talk on tumour growth. [ABSTRACT FROM AUTHOR]

Published

2019

8. Paths to expansion: Differential requirements of IRF4 in CD8+ T‐cell expansion driven by antigen and homeostatic cytokines.

Author

Lugli, Enrico, Brummelman, Jolanda, Pilipow, Karolina, and Roychoudhuri, Rahul

Abstract

Abstract: Interferon regulatory factor 4 (IRF4) regulates the clonal expansion and metabolic activity of activated T cells, but the precise context and mechanisms of its function in these processes are unclear. In this issue of the European Journal of Immunology, Miyakoda et al. [Eur. J. Immunol. 2018. 48: 1319–1328] show that IRF4 is required for activation and expansion of naïve and memory CD8+ T cells driven by T‐cell receptor (TCR) signaling, but dispensable for memory CD8+ T‐cell maintenance and homeostatic proliferation driven by homeostatic cytokines. The authors show that the function of IRF4 in CD8+ T‐cell expansion is partially dependent upon activation of the PI3K/AKT pathway through direct or indirect attenuation of PTEN expression. These data shed light upon the differential intracellular pathways required for naïve and memory T cells to respond to self‐antigens and/or homeostatic cytokines, and highlight the potential translational relevance of these findings in the context of immune reconstitution such as following allogeneic stem cell transplantation. [ABSTRACT FROM AUTHOR]

Published

2018

9. Regulatory T cells in cancer: where are we now?

Author

Gallimore, Awen, Quezada, Sergio A., and Roychoudhuri, Rahul

Subjects

CANCER cells, T cells, BIOLOGY

Abstract

Summary: There have been substantial strides forward in our understanding of the contribution of regulatory T (Treg) cells to cancer immunosuppression. In this issue, we present a series of papers highlighting emerging themes on this topic relevant not only to our understanding of the fundamental biology of tumour immunosuppression but also to the design of new immunotherapeutic approaches. The substantially shared biology of CD4+ conventional T (Tconv) and Treg cells necessitates a detailed understanding of the potentially opposing functional consequences that immunotherapies will have on Treg and Tconv cells, a prominent example being the potential for Treg‐mediated hyperprogressive disease following anti‐PD‐1 therapy. Such understanding will aid patient stratification and the rational design of combination therapies. It is also becoming clear, however, that Treg cells within tumours exhibit distinct biological features to both Tconv cells and Treg cells in other tissues. These distinct features provide the opportunity for development of targeted immunotherapies with greater efficacy and reduced potential for inducing systemic toxicity. [ABSTRACT FROM AUTHOR]

Published

2019

10. Ionic immune suppression within the tumour microenvironment limits T cell effector function.

Author

Eil, Robert, Vodnala, Suman K., Clever, David, Klebanoff, Christopher A., Sukumar, Madhusudhanan, Pan, Jenny H., Palmer, Douglas C., Gros, Alena, Yamamoto, Tori N., Patel, Shashank J., Guittard, Geoffrey C., Yu, Zhiya, Carbonaro, Valentina, Okkenhaug, Klaus, Schrump, David S., Linehan, W. Marston, Roychoudhuri, Rahul, and Restifo, Nicholas P.

Published

2016

11. The kinase DYRK1A reciprocally regulates the differentiation of Th17 and regulatory T cells.

Author

Khor, Bernard, Gagnon, John D., Goel, Gautam, Roche, Marly I., Conway, Kara L., Tran, Khoa, Aldrich, Leslie N., Sundberg, Thomas B., Paterson, Alison M., Mordecai, Scott, Dombkowski, David, Schirmer, Melanie, Tan, Pauline H., Bhan, Atul K., Roychoudhuri, Rahul, Restifo, Nicholas P., O'Shea, John J., Medoff, Benjamin D., Shamji, Alykhan F., and Schreiber, Stuart L.

Subjects

TYROSINE, PHOSPHORYLATION, CHEMICAL biology

Abstract

The article presents a study identifying a novel role for the dual specificity tyrosinephosphorylation-regulated kinase DYRK1A in regulating the balance with the use of an unbiased chemical biology approach.

Published

2015

12. Super-enhancers delineate disease-associated regulatory nodes in T cells.

Author

Vahedi, Golnaz, Kanno, Yuka, Furumoto, Yasuko, Jiang, Kan, Parker, Stephen C. J., Erdos, Michael R., Davis, Sean R., Roychoudhuri, Rahul, Restifo, Nicholas P., Gadina, Massimo, Tang, Zhonghui, Ruan, Yijun, Collins, Francis S., Sartorelli, Vittorio, and O'Shea, John J.

Subjects

T cells, GENE enhancers, GENE expression, GENETIC disorders, AUTOIMMUNITY, CYTOKINE receptors, JANUS kinases, GENETICS of rheumatoid arthritis

Abstract

Enhancers regulate spatiotemporal gene expression and impart cell-specific transcriptional outputs that drive cell identity. Super-enhancers (SEs), also known as stretch-enhancers, are a subset of enhancers especially important for genes associated with cell identity and genetic risk of disease. CD4+ T cells are critical for host defence and autoimmunity. Here we analysed maps of mouse T-cell SEs as a non-biased means of identifying key regulatory nodes involved in cell specification. We found that cytokines and cytokine receptors were the dominant class of genes exhibiting SE architecture in T cells. Nonetheless, the locus encoding Bach2, a key negative regulator of effector differentiation, emerged as the most prominent T-cell SE, revealing a network in which SE-associated genes critical for T-cell biology are repressed by BACH2. Disease-associated single-nucleotide polymorphisms for immune-mediated disorders, including rheumatoid arthritis, were highly enriched for T-cell SEs versus typical enhancers or SEs in other cell lineages. Intriguingly, treatment of T cells with the Janus kinase (JAK) inhibitor tofacitinib disproportionately altered the expression of rheumatoid arthritis risk genes with SE structures. Together, these results indicate that genes with SE architecture in T cells encompass a variety of cytokines and cytokine receptors but are controlled by a 'guardian' transcription factor, itself endowed with an SE. Thus, enumeration of SEs allows the unbiased determination of key regulatory nodes in T cells, which are preferentially modulated by pharmacological intervention. [ABSTRACT FROM AUTHOR]

Published

2015

13. Identification of the Genomic Insertion Site of Pmel-1 TCR α and β Transgenes by Next-Generation Sequencing.

Author

Ji, Yun, Abrams, Natalie, Zhu, Wei, Salinas, Eddie, Yu, Zhiya, Palmer, Douglas C., Jailwala, Parthav, Franco, Zulmarie, Roychoudhuri, Rahul, Stahlberg, Eric, Gattinoni, Luca, and Restifo, Nicholas P.

Subjects

TRANSGENES, TUMOR immunology, IMMUNOTHERAPY, AUTOIMMUNITY, CD8 antigen, T cell differentiation

Abstract

The pmel-1 T cell receptor transgenic mouse has been extensively employed as an ideal model system to study the mechanisms of tumor immunology, CD8+ T cell differentiation, autoimmunity and adoptive immunotherapy. The ‘zygosity’ of the transgene affects the transgene expression levels and may compromise optimal breeding scheme design. However, the integration sites for the pmel-1 mouse have remained uncharacterized. This is also true for many other commonly used transgenic mice created before the modern era of rapid and inexpensive next-generation sequencing. Here, we show that whole genome sequencing can be used to determine the exact pmel-1 genomic integration site, even with relatively ‘shallow’ (8X) coverage. The results were used to develop a validated polymerase chain reaction-based genotyping assay. For the first time, we provide a quick and convenient polymerase chain reaction method to determine the dosage of pmel-1 transgene for this freely and publically available mouse resource. We also demonstrate that next-generation sequencing provides a feasible approach for mapping foreign DNA integration sites, even when information of the original vector sequences is only partially known. [ABSTRACT FROM AUTHOR]

Published

2014

14. BACH2 represses effector programs to stabilize Treg-mediated immune homeostasis.

Author

Roychoudhuri, Rahul, Hirahara, Kiyoshi, Mousavi, Kambiz, Clever, David, Klebanoff, Christopher A., Bonelli, Michael, Sciumè, Giuseppe, Zare, Hossein, Vahedi, Golnaz, Dema, Barbara, Yu, Zhiya, Liu, Hui, Takahashi, Hayato, Rao, Mahadev, Muranski, Pawel, Crompton, Joseph G., Punkosdy, George, Bedognetti, Davide, Wang, Ena, and Hoffmann, Victoria

Subjects

AUTOIMMUNE diseases, HOMEOSTASIS, ASTHMA, CROHN'S disease, TRANSCRIPTION factors, T cells, GENETIC polymorphisms, MULTIPLE sclerosis

Abstract

Through their functional diversification, distinct lineages of CD4+ T cells can act to either drive or constrain immune-mediated pathology. Transcription factors are critical in the generation of cellular diversity, and negative regulators antagonistic to alternate fates often act in conjunction with positive regulators to stabilize lineage commitment. Genetic polymorphisms within a single locus encoding the transcription factor BACH2 are associated with numerous autoimmune and allergic diseases including asthma, Crohn's disease, coeliac disease, vitiligo, multiple sclerosis and type 1 diabetes. Although these associations point to a shared mechanism underlying susceptibility to diverse immune-mediated diseases, a function for BACH2 in the maintenance of immune homeostasis has not been established. Here, by studying mice in which the Bach2 gene is disrupted, we define BACH2 as a broad regulator of immune activation that stabilizes immunoregulatory capacity while repressing the differentiation programs of multiple effector lineages in CD4+ T cells. BACH2 was required for efficient formation of regulatory (Treg) cells and consequently for suppression of lethal inflammation in a manner that was Treg-cell-dependent. Assessment of the genome-wide function of BACH2, however, revealed that it represses genes associated with effector cell differentiation. Consequently, its absence during Treg polarization resulted in inappropriate diversion to effector lineages. In addition, BACH2 constrained full effector differentiation within TH1, TH2 and TH17 cell lineages. These findings identify BACH2 as a key regulator of CD4+ T-cell differentiation that prevents inflammatory disease by controlling the balance between tolerance and immunity. [ABSTRACT FROM AUTHOR]

Published

2013

15. Single-cell gene-expression profiling reveals qualitatively distinct CD8 I cells elicited by different gene-based vaccines.

Author

FIatz, Lukas, Roychoudhuri, Rahul, Honda, Mitsuo, Filali-Mouhim, Abdelali, Goulet, Jean-Philippe, Kettaf, Nadia, Lin, Min, Roederer, Mario, Haddad, Elias K., Sékaly, Rafick P., and Nabel, Gary J.

Subjects

DNA vaccines, GENE expression, IMMUNOPHENOTYPING, IMMUNE response, DNA microarrays, LEISHMANIA, INTERLEUKINS, T cells

Abstract

CD8 T cells play a key role in mediating protective immunity against selected pathogens after vaccination. Understanding the mechanism of this protection is dependent upon definition of the heterogeneity and complexity of cellular immune responses generated by different vaccines. Here, we identify previously unrecognized subsets of CD8 T cells based upon analysis of gene-expression patterns within single cells and show that they are differentially induced by different vaccines. Three prime-boost vector combinations encoding HIV Env stimulated antigen-specific CD8 T-cell populations of similar magnitude, phenotype, and functionality. Remarkably, however, analysis of single-cell gene-expression profiles enabled discrimination of a majority of central memory (CM) and effector memory (EM) CD8 T cells elicited by the three vaccines. Subsets of T cells could be defined based on their expression of Eomes, Cxcr3, and Ccrl, or Kirki, Kirgi, and CcrS in CM and EM cells, respectively, Of CM cells elicited by DNA prime-recombinant adenoviral (rAd) boost vectors, 67% were Eomes Ccrr Cxcr3, in contrast to only 7% and 2% stimulated by rAcl5-rAd5 or rAd-LCMV, respectively, Of EM cells elicited by DNArAd, 74% were KIrkl K!rgrCcr5T compared with only 26% and 20% for rAd5-rAd5 or rAd5-LCMV. Definition by single-cell gene profiling of specific CM and EM CD8 T-cell subsets that are differentially induced by different gene-based vaccines will facilitate the design and evaluation of vaccines, as well as enable our understanding of mechanisms of protective immunity. [ABSTRACT FROM AUTHOR]

Published

2011

16. Season of cancer diagnosis exerts distinct effects upon short- and long-term survival.

Author

Roychoudhuri, Rahul, Robinson, David, Coupland, Victoria, Holmberg, Lars, and Møller, Henrik

Abstract

Several epidemiological studies have shown an association between the season in which certain cancers are diagnosed and survival, with diagnosis in summer and autumn being associated with better survival. In this study, we have added resolution to the analysis of seasonality in cancer survival by considering mortality within several nonoverlapping time periods following diagnosis, thereby quantifying the separate contributions of mechanisms operating in the short term and in the longer term. We found evidence of seasonality acting on mortality within 2 distinct periods following diagnosis. Diagnosis in the summer was associated with substantially decreased mortality within the first month of diagnosis compared with winter in men with prostate cancer, those of both sexes with colorectal or lung cancer, and most strikingly, amongst women with breast cancer (hazard ratio 0.81 [95% confidence interval 0.75-0.86]). Adjusting for monthly variations in general mortality greatly attenuated the seasonal effects on short-term mortality. At long-term follow-up (>5 years), there was a consistent shift in the seasonality pattern, with autumn diagnosis alone being associated with decreased mortality, both in female breast cancer cases and in lung cancer cases of both sexes. We conclude that the higher survival observed amongst patients diagnosed in summer and autumn is predominantly a short-term phenomenon that is largely attributable to generally higher mortality in winter. However, the distinct mortality reduction observed in the long term amongst those diagnosed in the autumn, especially amongst breast cancer patients, may indicate the presence of a seasonally variable protective mechanism. © 2008 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2009

17. Increased cardiovascular mortality more than fifteen years after radiotherapy for breast cancer: a population-based study.

Author

Roychoudhuri, Rahul, Robinson, David, Putcha, Venkata, Cuzick, Jack, Darby, Sarah, and Møller, Henrik

Subjects

BREAST cancer, CARDIOVASCULAR diseases, RADIOTHERAPY complications, CANCER in women, ONCOLOGY

Abstract

Background: Breast radiotherapy as practised in the 1970s and 1980s resulted in significant myocardial exposure, and this was higher when the left breast was treated. It has been proposed that this difference might result in greater cardiovascular mortality following irradiation of the left breast when compared with the right. Methods: All cases of female breast cancer diagnosed between 1971 and 1988 and recorded on the Thames Cancer Registry database were followed up to the end of 2003 to identify cases who had died from ischaemic heart disease (IHD) or any cardiovascular disease (CVD). A proportional hazards regression analysis was performed, stratified by time since diagnosis, using as the baseline group those women with right-sided disease who did not receive radiotherapy, and adjusting for age at diagnosis. Results: A total of 20,871 women with breast cancer were included in the analysis, of which 51% had left-sided disease. Mortality at 15+ years after diagnosis was increased in recipients of left-breast radiotherapy compared to non-irradiated women with right-sided breast cancer, both for IHD (hazard ratio 1.59; 95% confidence interval 1.21-2.08; p = 0.001) and all CVD(hazard ratio 1.27; 95% confidence interval 1.07-1.51; p = 0.006). When irradiated women with left-sided breast cancer were compared with irradiated women with right-sided breast cancer, cardiovascular mortality at 15+ years after diagnosis was raised by around 25% (IHD: hazard ratio 1.23; 95% confidence interval 0.95-1.60; p = 0.114; CVD: hazard ratio 1.25; 95% confidence interval 1.05-1.49; p = 0.014). Conclusion: We have found an elevation in cardiovascular mortality more than 15 years after breast radiotherapy in women diagnosed with breast cancer between 1971 and 1988. The risk was greater following irradiation of the left breast compared with the right. This confirms that radiotherapy as practised in the 1970s and 1980s has resulted in significant long-term cardiac toxicity. In absolute terms, the increase in cardiovascular mortality induced by radiotherapy may be substantial, as these mortality events are relatively common. [ABSTRACT FROM AUTHOR]

Published

2007

18. Cancer survival is dependent on season of diagnosis and sunlight exposure.

Author

Lim, Hyun-Sook, Roychoudhuri, Rahul, Peto, Julian, Schwartz, Gary, Baade, Peter, and Møller, Henrik

Abstract

Sunlight is essential for the production of vitamin D in the body. Evidence exists to suggest that vitamin D metabolites may have a role in tumor growth suppression. In this large study, involving over a million cancer patients from the United Kingdom, we have analyzed the role of season of diagnosis and sunlight exposure in cancer survival for cancers of the breast, colorectum, lung, prostate and at all sites combined. We used population-based data from the Thames Cancer Registry to analyze cancer survival in periods 0-1 and 0-5 years after diagnosis. The analysis was performed using Cox proportional regression analysis adjusting for age and period at diagnosis and including season of diagnosis and sunlight exposure in the preceding months as factors in the analysis. We found evidence of substantial seasonality in cancer survival, with diagnosis in summer and autumn associated with improved survival compared with that in winter, especially in female breast cancer patients and both male and female lung cancer patients (hazard ratios 0.86 [95% CI 0.83-0.89], 0.95 [95% CI 0.92-0.97] and 0.95 [95% CI 0.93-0.98] respectively). Cumulative sunlight exposure in the months preceding diagnosis was also a predictor of subsequent survival, although season of diagnosis was a stronger predictor than cumulative sunlight exposure. We found seasonality in cancer survival to be stronger in women than in men. Our results add to a growing body of evidence that vitamin D metabolites play an important role in cancer survival. © 2006 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2006

19. A cell-based bioluminescence assay reveals dose-dependent and contextual repression of AP-1-driven gene expression by BACH2.

Author

Vardaka, Panagiota, Lozano, Teresa, Bot, Christopher, Ellery, Jonathan, Whiteside, Sarah K., Imianowski, Charlotte J., Farrow, Stuart, Walker, Simon, Okkenhaug, Hanneke, Yang, Jie, Okkenhaug, Klaus, Kuo, Paula, and Roychoudhuri, Rahul

Subjects

BIOLUMINESCENCE, GENE expression, TETRACYCLINE, LUCIFERASES, DRUG development

Abstract

Whereas effector CD4+ and CD8+ T cells promote immune activation and can drive clearance of infections and cancer, CD4+ regulatory T (Treg) cells suppress their function, contributing to both immune homeostasis and cancer immunosuppression. The transcription factor BACH2 functions as a pervasive regulator of T cell differentiation, promoting development of CD4+ Treg cells and suppressing the effector functions of multiple effector T cell (Teff) lineages. Here, we report the development of a stable cell-based bioluminescence assay of the transcription factor activity of BACH2. Tetracycline-inducible BACH2 expression resulted in suppression of phorbol 12-myristate 13-acetate (PMA)/ionomycin-driven activation of a luciferase reporter containing BACH2/AP-1 target sequences from the mouse Ifng + 18k enhancer. BACH2 expression repressed the luciferase signal in a dose-dependent manner but this activity was abolished at high levels of AP-1 signalling, suggesting contextual regulation of AP-1 driven gene expression by BACH2. Finally, using the reporter assay developed, we find that the histone deacetylase 3 (HDAC3)-selective inhibitor, RGFP966, inhibits BACH2-mediated repression of signal-driven luciferase expression. In addition to enabling mechanistic studies, this cell-based reporter may enable identification of small molecule agonists or antagonists of BACH2 function for drug development. [ABSTRACT FROM AUTHOR]

Published

2020

20. T cell stemness and dysfunction in tumors are triggered by a common mechanism.

Author

Vodnala, Suman Kumar, Eil, Robert, Kishton, Rigel J., Sukumar, Madhusudhanan, Yamamoto, Tori N., Ha, Ngoc-Han, Lee, Ping-Hsien, Shin, MinHwa, Patel, Shashank J., Yu, Zhiya, Palmer, Douglas C., Kruhlak, Michael J., Liu, Xiaojing, Locasale, Jason W., Huang, Jing, Roychoudhuri, Rahul, Finkel, Toren, Klebanoff, Christopher A., and Restifo, Nicholas P.

Published

2019

21. Oncogenic PI3Kα promotes multipotency in breast epithelial cells.

Author

Okkenhaug, Klaus and Roychoudhuri, Rahul

Published

2015