Your search keyword '"Monokine"' showing total 21 results

1. Chimeric antigen receptor macrophages (CAR-M) sensitize HER2+ solid tumors to PD1 blockade in pre-clinical models.

Author

Pierini, Stefano, Gabbasov, Rashid, Oliveira-Nunes, Maria Cecilia, Qureshi, Rehman, Worth, Alison, Huang, Shuo, Nagar, Karan, Griffin, Crystal, Lian, Lurong, Yashiro-Ohtani, Yumi, Ross, Kayleigh, Sloas, Christopher, Ball, Michael, Schott, Benjamin, Sonawane, Poonam, Cornell, Linara, Blumenthal, Daniel, Chhum, Sotheavy, Minutolo, Nicholas, and Ciccaglione, Kerri

Abstract

We previously developed human CAR macrophages (CAR-M) and demonstrated redirection of macrophage anti-tumor function leading to tumor control in immunodeficient xenograft models. Here, we develop clinically relevant fully immunocompetent syngeneic models to evaluate the potential for CAR-M to remodel the tumor microenvironment (TME), induce T cell anti-tumor immunity, and sensitize solid tumors to PD1/PDL1 checkpoint inhibition. In vivo, anti-HER2 CAR-M significantly reduce tumor burden, prolong survival, remodel the TME, increase intratumoral T cell and natural killer (NK) cell infiltration, and induce antigen spreading. CAR-M therapy protects against antigen-negative relapses in a T cell dependent fashion, confirming long-term anti-tumor immunity. In HER2+ solid tumors with limited sensitivity to anti-PD1 (aPD1) monotherapy, the combination of CAR-M and aPD1 significantly improves tumor growth control, survival, and remodeling of the TME in pre-clinical models. These results demonstrate synergy between CAR-M and T cell checkpoint blockade and provide a strategy to potentially enhance response to aPD1 therapy for patients with non-responsive tumors.Anti-PD1 monotherapy shows limited efficacy against HER2+ tumors. Here, the authors show that murine CAR macrophages (CAR-M) induce tumor microenvironment remodeling, T-cell mediated immunity and synergy with PD1 blockade, improving survival in immunocompetent female-mouse models of HER2+ solid tumors. [ABSTRACT FROM AUTHOR]

Published

2025

2. IFNγ-IL12 axis regulates intercellular crosstalk in metabolic dysfunction-associated steatotic liver disease.

Author

Friedline, Randall H., Noh, Hye Lim, Suk, Sujin, Albusharif, Mahaa, Dagdeviren, Sezin, Saengnipanthkul, Suchaorn, Kim, Bukyung, Kim, Allison M., Kim, Lauren H., Tauer, Lauren A., Baez Torres, Natalie M., Choi, Stephanie, Kim, Bo-Yeon, Rao, Suryateja D., Kasina, Kaushal, Sun, Cheng, Toles, Benjamin J., Zhou, Chan, Li, Zixiu, and Benoit, Vivian M.

Subjects

LIVER diseases, HEPATIC fibrosis, FIBROBLAST growth factors, HEPATITIS, INSULIN resistance, FATTY liver, INSULIN

Abstract

Obesity is a major cause of metabolic dysfunction-associated steatohepatitis (MASH) and is characterized by inflammation and insulin resistance. Interferon-γ (IFNγ) is a pro-inflammatory cytokine elevated in obesity and modulating macrophage functions. Here, we show that male mice with loss of IFNγ signaling in myeloid cells (Lyz-IFNγR2−/−) are protected from diet-induced insulin resistance despite fatty liver. Obesity-mediated liver inflammation is also attenuated with reduced interleukin (IL)−12, a cytokine primarily released by macrophages, and IL-12 treatment in vivo causes insulin resistance by impairing hepatic insulin signaling. Following MASH diets, Lyz-IFNγR2−/− mice are rescued from developing liver fibrosis, which is associated with reduced fibroblast growth factor (FGF) 21 levels. These results indicate critical roles for IFNγ signaling in macrophages and their release of IL-12 in modulating obesity-mediated insulin resistance and fatty liver progression to MASH. In this work, we identify the IFNγ-IL12 axis in regulating intercellular crosstalk in the liver and as potential therapeutic targets to treat MASH. Metabolic liver disease is highly prevalent in subjects with obesity and involves inflammation, insulin resistance, and fibrosis, leading to cirrhosis. Here, the authors show the IFNγ-IL12 axis in regulating intercellular crosstalk in the liver and playing a major role in the pathogenesis of metabolic liver disease. [ABSTRACT FROM AUTHOR]

Published

2024

3. Inflammatory and neurodegenerative serum protein biomarkers increase sensitivity to detect clinical and radiographic disease activity in multiple sclerosis.

Author

Chitnis, Tanuja, Qureshi, Ferhan, Gehman, Victor M., Becich, Michael, Bove, Riley, Cree, Bruce A. C., Gomez, Refujia, Hauser, Stephen L., Henry, Roland G., Katrib, Amal, Lokhande, Hrishikesh, Paul, Anu, Caillier, Stacy J., Santaniello, Adam, Sattarnezhad, Neda, Saxena, Shrishti, Weiner, Howard, Hajime Yano, and Baranzini, Sergio E.

Abstract

The multifaceted nature of multiple sclerosis requires quantitative biomarkers that can provide insights related to diverse physiological pathways. To this end, proteomic analysis of deeply-phenotyped serum samples, biological pathway modeling, and network analysis were performed to elucidate inflammatory and neurodegenerative processes, identifying sensitive biomarkers of multiple sclerosis disease activity. Here, we evaluated the concentrations of > 1400 serum proteins in 630 samples from three multiple sclerosis cohorts for association with clinical and radiographic new disease activity. Twenty proteins were associated with increased clinical and radiographic multiple sclerosis disease activity for inclusion in a custom assay panel. Serum neurofilament light chain showed the strongest univariate correlation with gadolinium lesion activity, clinical relapse status, and annualized relapse rate. Multivariate modeling outperformed univariate for all endpoints. A comprehensive biomarker panel including the twenty proteins identified in this study could serve to characterize disease activity for a patient with multiple sclerosis. [ABSTRACT FROM AUTHOR]

Published

2024

4. Immunotherapy targeting different immune compartments in combination with radiation therapy induces regression of resistant tumors.

Author

Rudqvist, Nils-Petter, Charpentier, Maud, Lhuillier, Claire, Wennerberg, Erik, Spada, Sheila, Sheridan, Caroline, Zhou, Xi Kathy, Zhang, Tuo, Formenti, Silvia C., Sims, Jennifer S., Alonso, Alicia, and Demaria, Sandra

Subjects

T cells, T helper cells, RADIOTHERAPY, REGULATORY T cells, IMMUNE checkpoint inhibitors, TRIPLE-negative breast cancer, PROGRAMMED cell death 1 receptors, BREAST

Abstract

Radiation therapy (RT) increases tumor response to CTLA-4 inhibition (CTLA4i) in mice and in some patients, yet deep responses are rare. To identify rational combinations of immunotherapy to improve responses we use models of triple negative breast cancer highly resistant to immunotherapy in female mice. We find that CTLA4i promotes the expansion of CD4+ T helper cells, whereas RT enhances T cell clonality and enriches for CD8+ T cells with an exhausted phenotype. Combination therapy decreases regulatory CD4+ T cells and increases effector memory, early activation and precursor exhausted CD8+ T cells. A combined gene signature comprising these three CD8+ T cell clusters is associated with survival in patients. Here we show that targeting additional immune checkpoints expressed by intratumoral T cells, including PD1, is not effective, whereas CD40 agonist therapy recruits resistant tumors into responding to the combination of RT and CTLA4i, indicating the need to target different immune compartments. Radiation therapy (RT) has been shown to improve responses to immunotherapy in preclinical cancer models, but deep responses in patients are still rare. Here the authors provide immunological insights into the response to RT and CTLA4 inhibition in tumor bearing mice and show that agonistic CD40 therapy improves response to the combination of RT and immune checkpoint inhibition. [ABSTRACT FROM AUTHOR]

Published

2023

5. Abrupt perturbation and delayed recovery of the vaginal ecosystem following childbirth.

Author

Costello, Elizabeth K., DiGiulio, Daniel B., Robaczewska, Anna, Symul, Laura, Wong, Ronald J., Shaw, Gary M., Stevenson, David K., Holmes, Susan P., Kwon, Douglas S., and Relman, David A.

Subjects

DELIVERY (Obstetrics), CHILDBIRTH, REPRODUCTIVE health, BIRTH rate, PUERPERIUM, ECOSYSTEMS, BACTERIAL communities

Abstract

The vaginal ecosystem is closely tied to human health and reproductive outcomes, yet its dynamics in the wake of childbirth remain poorly characterized. Here, we profile the vaginal microbiota and cytokine milieu of participants sampled longitudinally throughout pregnancy and for at least one year postpartum. We show that delivery, regardless of mode, is associated with a vaginal pro-inflammatory cytokine response and the loss of Lactobacillus dominance. By contrast, neither the progression of gestation nor the approach of labor strongly altered the vaginal ecosystem. At 9.5-months postpartum—the latest timepoint at which cytokines were assessed—elevated inflammation coincided with vaginal bacterial communities that had remained perturbed (highly diverse) from the time of delivery. Time-to-event analysis indicated a one-year postpartum probability of transitioning to Lactobacillus dominance of 49.4%. As diversity and inflammation declined during the postpartum period, dominance by L. crispatus, the quintessential health-associated commensal, failed to return: its prevalence before, immediately after, and one year after delivery was 41%, 4%, and 9%, respectively. Revisiting our pre-delivery data, we found that a prior live birth was associated with a lower odds of L. crispatus dominance in pregnant participants—an outcome modestly tempered by a longer (> 18-month) interpregnancy interval. Our results suggest that reproductive history and childbirth in particular remodel the vaginal ecosystem and that the timing and degree of recovery from delivery may help determine the subsequent health of the woman and of future pregnancies. Childbirth prompts a vaginal inflammatory response and loss of Lactobacillus dominance. This disturbance, the authors show, reverberates deep into the first postpartum year, with evidence of recovery in only 49% of women by year's end. [ABSTRACT FROM AUTHOR]

Published

2023

6. Multi-omic brain and behavioral correlates of cell-free fetal DNA methylation in macaque maternal obesity models.

Author

Laufer, Benjamin I., Hasegawa, Yu, Zhang, Zhichao, Hogrefe, Casey E., Del Rosso, Laura A., Haapanen, Lori, Hwang, Hyeyeon, Bauman, Melissa D., Van de Water, Judy, Taha, Ameer Y., Slupsky, Carolyn M., Golub, Mari S., Capitanio, John P., VandeVoort, Catherine A., Walker, Cheryl K., and LaSalle, Janine M.

Subjects

CELL-free DNA, DNA methylation, TRANSCRIPTION factors, CIRCULATING tumor DNA, MACAQUES, OBESITY, RHESUS monkeys

Abstract

Maternal obesity during pregnancy is associated with neurodevelopmental disorder (NDD) risk. We utilized integrative multi-omics to examine maternal obesity effects on offspring neurodevelopment in rhesus macaques by comparison to lean controls and two interventions. Differentially methylated regions (DMRs) from longitudinal maternal blood-derived cell-free fetal DNA (cffDNA) significantly overlapped with DMRs from infant brain. The DMRs were enriched for neurodevelopmental functions, methylation-sensitive developmental transcription factor motifs, and human NDD DMRs identified from brain and placenta. Brain and cffDNA methylation levels from a large region overlapping mir-663 correlated with maternal obesity, metabolic and immune markers, and infant behavior. A DUX4 hippocampal co-methylation network correlated with maternal obesity, infant behavior, infant hippocampal lipidomic and metabolomic profiles, and maternal blood measurements of DUX4 cffDNA methylation, cytokines, and metabolites. We conclude that in this model, maternal obesity was associated with changes in the infant brain and behavior, and these differences were detectable in pregnancy through integrative analyses of cffDNA methylation with immune and metabolic factors. In animal models, maternal obesity is associated with development of neurodevelopmental disorder like phenotypes. Here the authors show in a macaque model that in obese dams, cell-free fetal DNA methylation, inflammatory cytokines, and metabolites correlated with infant brain DNA methylation, lipids, and metabolites. [ABSTRACT FROM AUTHOR]

Published

2022

7. Mesenchymal stem cells transfer mitochondria to allogeneic Tregs in an HLA-dependent manner improving their immunosuppressive activity.

Author

Piekarska, Karolina, Urban-Wójciuk, Zuzanna, Kurkowiak, Małgorzta, Pelikant-Małecka, Iwona, Schumacher, Adriana, Sakowska, Justyna, Spodnik, Jan Henryk, Arcimowicz, Łukasz, Zielińska, Hanna, Tymoniuk, Bogusław, Renkielska, Alicja, Siebert, Janusz, Słomińska, Ewa, Trzonkowski, Piotr, Hupp, Ted, and Marek-Trzonkowska, Natalia Maria

Subjects

MESENCHYMAL stem cells, REGULATORY T cells, T cells, LYMPHOCYTE subsets, CELL populations, PROGENITOR cells

Abstract

Cell-based immunotherapies can provide safe and effective treatments for various disorders including autoimmunity, cancer, and excessive proinflammatory events in sepsis or viral infections. However, to achieve this goal there is a need for deeper understanding of mechanisms of the intercellular interactions. Regulatory T cells (Tregs) are a lymphocyte subset that maintain peripheral tolerance, whilst mesenchymal stem cells (MSCs) are multipotent nonhematopoietic progenitor cells. Despite coming from different origins, Tregs and MSCs share immunoregulatory properties that have been tested in clinical trials. Here we demonstrate how direct and indirect contact with allogenic MSCs improves Tregs' potential for accumulation of immunosuppressive adenosine and suppression of conventional T cell proliferation, making them more potent therapeutic tools. Our results also demonstrate that direct communication between Tregs and MSCs is based on transfer of active mitochondria and fragments of plasma membrane from MSCs to Tregs, an event that is HLA-dependent and associates with HLA-C and HLA-DRB1 eplet mismatch load between Treg and MSC donors. Regulatory T (Treg) cells and mesenchymal stem cells (MSCs) are both cell populations capable of immune tolerance induction. Here the authors show that the transfer of mitochondria from mesenchymal stem cells to allogeneic Treg cells in an HLA-dependent manner results in enhanced immunosuppressive functions of Treg cells. [ABSTRACT FROM AUTHOR]

Published

2022

8. Biomimetic nanoparticles deliver mRNAs encoding costimulatory receptors and enhance T cell mediated cancer immunotherapy.

Author

Li, Wenqing, Zhang, Xinfu, Zhang, Chengxiang, Yan, Jingyue, Hou, Xucheng, Du, Shi, Zeng, Chunxi, Zhao, Weiyu, Deng, Binbin, McComb, David W., Zhang, Yuebao, Kang, Diana D., Li, Junan, Carson III, William E., and Dong, Yizhou

Subjects

T cell receptors, T cells, TUMOR-infiltrating immune cells, IMMUNOTHERAPY, CANCER cells, CYTOTOXIC T cells, CELL receptors

Abstract

Antibodies targeting costimulatory receptors of T cells have been developed for the activation of T cell immunity in cancer immunotherapy. However, costimulatory molecule expression is often lacking in tumor-infiltrating immune cells, which can impede antibody-mediated immunotherapy. Here, we hypothesize that delivery of costimulatory receptor mRNA to tumor-infiltrating T cells will enhance the antitumor effects of antibodies. We first design a library of biomimetic nanoparticles and find that phospholipid nanoparticles (PL1) effectively deliver costimulatory receptor mRNA (CD137 or OX40) to T cells. Then, we demonstrate that the combination of PL1-OX40 mRNA and anti-OX40 antibody exhibits significantly improved antitumor activity compared to anti-OX40 antibody alone in multiple tumor models. This treatment regimen results in a 60% complete response rate in the A20 tumor model, with these mice being resistant to rechallenge by A20 tumor cells. Additionally, the combination of PL1-OX40 mRNA and anti-OX40 antibody significantly boosts the antitumor immune response to anti-PD-1 + anti-CTLA-4 antibodies in the B16F10 tumor model. This study supports the concept of delivering mRNA encoding costimulatory receptors in combination with the corresponding agonistic antibody as a strategy to enhance cancer immunotherapy. Antibodies targeting OX40 or CD137, two T cell costimulatory receptors, have been shown to improve antitumor immunity. Here the authors design a phospholipid-derived nanoparticle to deliver OX40 or CD137 mRNA to T cells in vivo, improving efficacy of anti-OX40 and anti-CD137 antibody therapy in preclinical tumor models. [ABSTRACT FROM AUTHOR]

Published

2021

9. Tumour-targeted interleukin-12 and entinostat combination therapy improves cancer survival by reprogramming the tumour immune cell landscape.

Author

Hicks, Kristin C., Chariou, Paul L., Ozawa, Yohei, Minnar, Christine M., Knudson, Karin M., Meyer, Thomas J., Bian, Jing, Cam, Margaret, Schlom, Jeffrey, and Gameiro, Sofia R.

Subjects

INTERLEUKIN-12, IMMUNE checkpoint proteins, HISTONE deacetylase inhibitors, TUMOR microenvironment, OVERALL survival, T cells

Abstract

Poorly inflamed carcinomas do not respond well to immune checkpoint blockade. Converting the tumour microenvironment into a functionally inflamed immune hub would extend the clinical benefit of immune therapy to a larger proportion of cancer patients. Here we show, by using comprehensive single-cell transcriptome, proteome, and immune cell analysis, that Entinostat, a class I histone deacetylase inhibitor, facilitates accumulation of the necrosis-targeted recombinant murine immune-cytokine, NHS-rmIL12, in experimental mouse colon carcinomas and poorly immunogenic breast tumours. This combination therapy reprograms the tumour innate and adaptive immune milieu to an inflamed landscape, where the concerted action of highly functional CD8+ T cells and activated neutrophils drive macrophage M1-like polarization, leading to complete tumour eradication in 41.7%-100% of cases. Biomarker signature of favourable overall survival in multiple human tumor types shows close resemblance to the immune pattern generated by Entinostat/NHS-rmIL12 combination therapy. Collectively, these findings provide a rationale for combining NHS-IL12 with Entinostat in the clinical setting. The immunocytokine NHS-IL12 is targeted to necrotic tumour areas to prompt an immune response. Authors show here in mouse colon and breast models that the combination of histone deacetylase inhibitor, Entinostat, and NHS-IL12 generates a tumour microenvironment that favours tumour resolution. [ABSTRACT FROM AUTHOR]

Published

2021

10. Metastasis-initiating cells induce and exploit a fibroblast niche to fuel malignant colonization of the lungs.

Author

Pein, Maren, Insua-Rodríguez, Jacob, Hongu, Tsunaki, Riedel, Angela, Meier, Jasmin, Wiedmann, Lena, Decker, Kristin, Essers, Marieke A. G., Sinn, Hans-Peter, Spaich, Saskia, Sütterlin, Marc, Schneeweiss, Andreas, Trumpp, Andreas, and Oskarsson, Thordur

Subjects

CHEMOKINE receptors, CXCR4 receptors, CANCER cells, COLONIZATION, LUNGS, BREAST cancer, RESPIRATORY organs

Abstract

Metastatic colonization relies on interactions between disseminated cancer cells and the microenvironment in secondary organs. Here, we show that disseminated breast cancer cells evoke phenotypic changes in lung fibroblasts, forming a supportive metastatic niche. Colonization of the lungs confers an inflammatory phenotype in metastasis-associated fibroblasts. Specifically, IL-1α and IL-1β secreted by breast cancer cells induce CXCL9 and CXCL10 production in lung fibroblasts via NF-κB signaling, fueling the growth of lung metastases. Notably, we find that the chemokine receptor CXCR3, that binds CXCL9/10, is specifically expressed in a small subset of breast cancer cells, which exhibits tumor-initiating ability when co-transplanted with fibroblasts and has high JNK signaling that drives IL-1α/β expression. Importantly, disruption of the intercellular JNK-IL-1-CXCL9/10-CXCR3 axis reduces metastatic colonization in xenograft and syngeneic mouse models. These data mechanistically demonstrate an essential role for the molecular crosstalk between breast cancer cells and their fibroblast niche in the progression of metastasis. How cancer cells engage the microenvironment to establish metastasis is poorly understood. Here, the authors show that CXCR3-expressing breast cancer cells secrete IL-1 to induce a paracrine crosstalk with fibroblasts in the lung, which involves CXCL9/10 production and results in colonization of the lung. [ABSTRACT FROM AUTHOR]

Published

2020

11. Granulocyte-colony stimulating factor controls neural and behavioral plasticity in response to cocaine.

Author

Calipari, Erin S., Godino, Arthur, Peck, Emily G., Salery, Marine, Mervosh, Nicholas L., Landry, Joseph A., Russo, Scott J., Hurd, Yasmin L., Nestler, Eric J., and Kiraly, Drew D.

Subjects

GRANULOCYTE-colony stimulating factor, NEUROPLASTICITY, COCAINE abuse, COCAINE, GRANULOCYTES, NUCLEUS accumbens, PREFRONTAL cortex

Abstract

Cocaine addiction is characterized by dysfunction in reward-related brain circuits, leading to maladaptive motivation to seek and take the drug. There are currently no clinically available pharmacotherapies to treat cocaine addiction. Through a broad screen of innate immune mediators, we identify granulocyte-colony stimulating factor (G-CSF) as a potent mediator of cocaine-induced adaptations. Here we report that G-CSF potentiates cocaine-induced increases in neural activity in the nucleus accumbens (NAc) and prefrontal cortex. In addition, G-CSF injections potentiate cocaine place preference and enhance motivation to self-administer cocaine, while not affecting responses to natural rewards. Infusion of G-CSF neutralizing antibody into NAc blocks the ability of G-CSF to modulate cocaine’s behavioral effects, providing a direct link between central G-CSF action in NAc and cocaine reward. These results demonstrate that manipulating G-CSF is sufficient to alter the motivation for cocaine, but not natural rewards, providing a pharmacotherapeutic avenue to manipulate addictive behaviors without abuse potential. [ABSTRACT FROM AUTHOR]

Published

2018

12. Dual blockade of CD47 and HER2 eliminates radioresistant breast cancer cells.

Author

Candas-Green, Demet, Xie, Bowen, Huang, Jie, Fan, Ming, Wang, Aijun, Menaa, Cheikh, Zhang, Yanhong, Zhang, Lu, Jing, Di, Azghadi, Soheila, Zhou, Weibing, Liu, Lin, Jiang, Nian, Li, Tao, Gao, Tianyi, Sweeney, Colleen, Shen, Rulong, Lin, Tzu-yin, Pan, Chong-xian, and Ozpiskin, Omer M.

Subjects

CANCER cells, BREAST cancer, CANCER invasiveness, RECEPTOR antibodies, CANCER radiotherapy, PHAGOCYTOSIS

Abstract

Although the efficacy of cancer radiotherapy (RT) can be enhanced by targeted immunotherapy, the immunosuppressive factors induced by radiation on tumor cells remain to be identified. Here, we report that CD47-mediated anti-phagocytosis is concurrently upregulated with HER2 in radioresistant breast cancer (BC) cells and RT-treated mouse syngeneic BC. Co-expression of both receptors is more frequently detected in recurrent BC patients with poor prognosis. CD47 is upregulated preferentially in HER2-expressing cells, and blocking CD47 or HER2 reduces both receptors with diminished clonogenicity and augmented phagocytosis. CRISPR-mediated CD47 and HER2 dual knockouts not only inhibit clonogenicity but also enhance macrophage-mediated attack. Dual antibody of both receptors synergizes with RT in control of syngeneic mouse breast tumor. These results provide the evidence that aggressive behavior of radioresistant BC is caused by CD47-mediated anti-phagocytosis conjugated with HER2-prompted proliferation. Dual blockade of CD47 and HER2 is suggested to eliminate resistant cancer cells in BC radiotherapy. The emergence of tumour adaptive radioresistance can limit the success of radiation therapy and immunotherapy in breast cancer. In this study, the authors demonstrate that CD47 and HER2 are coordinating in tumor response to radiation and that co-blockage of both receptors can eliminate radiorestistant breast cancer cells. [ABSTRACT FROM AUTHOR]

Published

2020

13. HPV infection and the genital cytokine milieu in women at high risk of HIV acquisition.

Author

Liebenberg, Lenine J. P., McKinnon, Lyle R., Yende-Zuma, Nonhlanhla, Garrett, Nigel, Baxter, Cheryl, Kharsany, Ayesha B. M., Archary, Derseree, Rositch, Anne, Samsunder, Natasha, Mansoor, Leila E., Passmore, Jo-Ann S., Abdool Karim, Salim S., and Abdool Karim, Quarraisha

Subjects

HUMAN papillomavirus vaccines, CYTOKINES, HIV, COHORT analysis, INFLAMMATION

Abstract

Human papillomavirus (HPV) infection correlates with higher rates of HIV acquisition, but the underlying biological mechanisms are unclear. Here we study associations between HPV and HIV acquisition and relate these to vaginal cytokine profiles in an observational cohort of women at high risk of HIV infection (CAPRISA 004, n = 779) and with 74% HPV prevalence. We report here that HPV infection associates with a 2.5-fold increase in HIV acquisition risk in this population (95% CI: 1.2–5.3). Among 48 vaginal cytokines profiled, cytokines associated with HPV infection overlap substantially with cytokines associated with HIV risk, but are distinct from those observed in HPV negative women. Although our data do not establish a causative link between HPV status and the risk of HIV, we suggest that increasing HPV vaccination coverage may carry an additional benefit of reducing the risk of contracting HIV infection, particularly in regions with high HPV prevalence. Cervicovaginal inflammation and human papillomavirus (HPV) are separately associated with increased risk of HIV acquisition. Here the authors longitudinally profile 48 cervicovaginal cytokines and HPV status in a large observational HIV high-risk cohort, and show the same cytokines associate with HPV infection and HIV risk. [ABSTRACT FROM AUTHOR]

Published

2019

14. Time elapsed between Zika and dengue virus infections affects antibody and T cell responses.

Author

Pérez-Guzmán, Erick X., Pantoja, Petraleigh, Serrano-Collazo, Crisanta, Hassert, Mariah A., Ortiz-Rosa, Alexandra, Rodríguez, Idia V., Giavedoni, Luis, Hodara, Vida, Parodi, Laura, Cruz, Lorna, Arana, Teresa, White, Laura J., Martínez, Melween I., Weiskopf, Daniela, Brien, James D., de Silva, Aravinda, Pinto, Amelia K., and Sariol, Carlos A.

Subjects

ZIKA virus infections, T cells, VIRAL antibodies, INTERLEUKIN-21, DENGUE viruses, ZIKA virus, RHESUS monkeys, ARBOVIRUS diseases

Abstract

Zika virus (ZIKV) and dengue virus (DENV) are co-endemic in many parts of the world, but the impact of ZIKV infection on subsequent DENV infection is not well understood. Here we show in rhesus macaques that the time elapsed after ZIKV infection affects the immune response to DENV infection. We show that previous ZIKV exposure increases the magnitude of the antibody and T cell responses against DENV. The time interval between ZIKV and subsequent DENV infection further affects the immune response. A mid-convalescent period of 10 months after ZIKV infection results in higher and more durable antibody and T cell responses to DENV infection than a short period of 2 months. In contrast, previous ZIKV infection does not affect DENV viremia or pro-inflammatory status. Collectively, we find no evidence of a detrimental effect of ZIKV immunity in a subsequent DENV infection. This supports the implementation of ZIKV vaccines that could also boost immunity against future DENV epidemics. Here, the authors show that the time elapsed between Zika infection and subsequent dengue virus infection affects the magnitude and durability of the antibody and cell-mediated immune responses against dengue virus, but not viremia. This research in non-human primates has implications for co-endemic regions and vaccination. [ABSTRACT FROM AUTHOR]

Published

2019

15. Schistosoma mansoni treatment reduces HIV entry into cervical CD4+ T cells and induces IFN-I pathways.

Author

Yegorov, Sergey, Joag, Vineet, Galiwango, Ronald M., Good, Sara V., Mpendo, Juliet, Tannich, Egbert, Boggild, Andrea K., Kiwanuka, Noah, Bagaya, Bernard S., and Kaul, Rupert

Abstract

Schistosoma mansoni (Sm) infection has been linked with an increased risk of HIV acquisition in women. Therefore, defining the mechanism(s) by which Sm alters HIV susceptibility might lead to new HIV prevention strategies. Here, we analyze the impact of standard Sm therapy in HIV-uninfected Sm+ Ugandan adult women on genital HIV susceptibility and mucosal and systemic immunology. Schistosomiasis treatment induces a profound reduction of HIV entry into cervical and blood CD4+ T cells that is sustained for up to two months, despite transient systemic and mucosal immune activation and elevated genital IL-1α levels. Genital IFN-α2a levels are also elevated post-treatment, and IFN-α2a blocks HIV entry into primary CD4+ T cells ex vivo. Transcriptomic analysis of blood mononuclear cells post-Sm treatment shows IFN-I pathway up-regulation and partial reversal of Sm-dysregulated interferon signaling. These findings indicate that Sm therapy may reduce HIV susceptibility for women with Sm infection, potentially through de-repression of IFN-I pathways. Schistosoma mansoniinfection has been linked with an increased risk of HIV acquisition in women. Here, the authors show that standard S. mansoniinfection treatment causes a reduction of HIV entry into cervical and blood CD4+ T cells, which is sustained for up to two months and is associated with de-repression of IFN-I signaling. [ABSTRACT FROM AUTHOR]

Published

2019

16. Altered respiratory virome and serum cytokine profile associated with recurrent respiratory tract infections in children.

Author

Li, Yanpeng, Fu, Xuemin, Ma, Jinmin, Zhang, Jianhui, Hu, Yihong, Dong, Wei, Wan, Zhenzhou, Li, Qiongfang, Kuang, Yi-Qun, Lan, Ke, Jin, Xia, Wang, Jian-Hua, and Zhang, Chiyu

Abstract

Recurrent acute respiratory tract infections (ARTIs) affect a large population, yet the specific decisive factors are largely unknown. Here we study a population of 4407 children diagnosed with ARTI, comparing respiratory virome and serum cytokine profiles associated with multiple ARTIs and single ARTI during a six-year period. The relative abundance of Propionibacterium phages is significantly elevated in multiple ARTIs compared to single ARTI group. Serum levels of TIMP-1 and PDGF-BB are markedly increased in multiple ARTIs compared to single-ARTI and non-ARTI controls, making these two cytokines potential predictors for multiple ARTIs. The presence of Propionibacterium phages is associated with higher levels of TIMP-1 and PDGF-BB. Receiver operating characteristic (ROC) curve analyses show that the combination of TIMP-1, PDGF-BB and Propionibacterium phages could be a strong predictor for multiple ARTIs. These findings indicate that respiratory microbe homeostasis and specific cytokines are associated with the onset of multiple ARTIs over time. Here, the authors determine the respiratory virome and serum cytokine profile in children diagnosed with acute respiratory tract infections (ARTI) and show that relative abundance of Propionibacterium phages as well as serum levels of TIMP-1 and PDGF-BB are increased in multiple ARTIs compared with single ARTI. [ABSTRACT FROM AUTHOR]

Published

2019

17. Breakdown of adaptive immunotolerance induces hepatocellular carcinoma in HBsAg-tg mice.

Author

Zong, Lu, Peng, Hui, Sun, Cheng, Li, Fenglei, Zheng, Meijuan, Chen, Yongyan, Wei, Haiming, Sun, Rui, and Tian, Zhigang

Abstract

Hepatitis B virus (HBV) can induce chronic inflammation, cirrhosis, and eventually hepatocellular carcinoma (HCC). Despite evidence suggesting a link between adaptive immunity and HBV-related diseases in humans, the immunopathogenic mechanisms involved are seldom described. Here we show that expression of TIGIT, a promising immune checkpoint in tumor immunotherapy, increases with age on hepatic CD8+ T cells in HBsAg-transgenic (HBs-tg) mice whose adaptive immune system is tolerant to HBsAg. TIGIT blockade or deficiency leads to chronic hepatitis and fibrosis, along with the emergence of functional HBsAg-specific cytotoxic T lymphocytes (CTLs), suggesting adaptive immune tolerance could be broken by TIGIT blockade or deficiency. Importantly, HBsAg vaccination further induces nonresolving inflammation and HCC in a CD8+ T cell-dependent manner in TIGIT-blocked or -deficient HBs-tg mice. Therefore, CD8+ T cells play an important role in adaptive immunity-mediated tumor progression and TIGIT is critical in maintenance of liver tolerance by keeping CTLs in homeostatic balance. Chronic hepatitis B virus (HBV) infection is a risk factor for hepatocellular carcinoma (HCC) and is associated with immune tolerance to HBV. Here the authors show, in a transgenic mouse model, that rescuing T cells function via inhibition of co-inhibitory receptor TIGIT results in HCC development via supporting inflammation. [ABSTRACT FROM AUTHOR]

Published

2019

18. The immunoreceptor NKG2D promotes tumour growth in a model of hepatocellular carcinoma.

Author

Sheppard, Sam, Guedes, Joana, Mroz, Anna, Zavitsanou, Anastasia-Maria, Kudo, Hiromi, Rothery, Stephen M., Angelopoulos, Panagiotis, Goldin, Robert, and Guerra, Nadia

Published

2017

19. Osteoblasts secrete Cxcl9 to regulate angiogenesis in bone.

Author

Huang, Bin, Wang, Wenhao, Li, Qingchu, Wang, Zhenyu, Yan, Bo, Zhang, Zhongmin, Wang, Liang, Huang, Minjun, Jia, Chunhong, Lu, Jiansen, Liu, Sichi, Chen, Hongdong, Li, Mangmang, Cai, Daozhang, Jiang, Yu, Jin, Dadi, and Bai, Xiaochun

Published

2016

20. Inhibition of ROS and upregulation of inflammatory cytokines by FoxO3a promotes survival against Salmonella typhimurium.

Author

Joseph, Julie, Ametepe, Emmanuelle S., Haribabu, Naveen, Agbayani, Gerard, Krishnan, Lakshmi, Blais, Alexandre, and Sad, Subash

Published

2016

21. Early role of vascular dysregulation on late-onset Alzheimer's disease based on multifactorial data-driven analysis.

Author

Iturria-Medina, Y., Sotero, R. C., Toussaint, P. J., Mateos-Pérez, J. M., and Evans, A. C.

Published

2016