Gotowa bibliografia na temat „Immunity”
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Artykuły w czasopismach na temat "Immunity"
DH, Jha. "Immunity and Ayurveda". Journal of Natural & Ayurvedic Medicine 4, nr 2 (2.04.2020): 1. http://dx.doi.org/10.23880/jonam-16000248.
Pełny tekst źródła&NA;. "Immunity lost, immunity regained". Inpharma Weekly &NA;, nr 760 (październik 1990): 17. http://dx.doi.org/10.2165/00128413-199007600-00049.
Pełny tekst źródłaKhudhair, Abdulkareem Salman. "Herd Immunity or Community Immunity". Scholars Journal of Medical Case Reports 08, nr 04 (30.04.2020): 508–9. http://dx.doi.org/10.36347/sjmcr.2020.v08i04.026.
Pełny tekst źródłaCotter, S. C., i R. M. Kilner. "Personal immunity versus social immunity". Behavioral Ecology 21, nr 4 (4.06.2010): 663–68. http://dx.doi.org/10.1093/beheco/arq070.
Pełny tekst źródłaTakahashi, Hidemi. "Innate Immunity and Acqired Immunity". Journal of Nippon Medical School 69, nr 5 (2002): 410–14. http://dx.doi.org/10.1272/jnms.69.410.
Pełny tekst źródłaLee, Theodore M. "Immunity". Emerging Infectious Diseases 22, nr 4 (kwiecień 2016): 766. http://dx.doi.org/10.3201/eid2204.151858.
Pełny tekst źródłaWilkinson, Lise. "Immunity". Lancet 365, nr 9469 (kwiecień 2005): 1459. http://dx.doi.org/10.1016/s0140-6736(05)66405-7.
Pełny tekst źródłaReddy, Karthik, Moritz Schularick i Vasiliki Skreta. "IMMUNITY". International Economic Review 61, nr 2 (31.03.2020): 531–64. http://dx.doi.org/10.1111/iere.12433.
Pełny tekst źródłaMuske, Carol. "Immunity". Missouri Review 9, nr 1 (1985): 20–21. http://dx.doi.org/10.1353/mis.1985.0140.
Pełny tekst źródłaLewin, Benjamin. "Immunity". Immunity 1, nr 1 (kwiecień 1994): 1. http://dx.doi.org/10.1016/1074-7613(94)90002-7.
Pełny tekst źródłaRozprawy doktorskie na temat "Immunity"
Daneshvar, Fatemeh. "L’immunité juridictionnelle des États et des organismes d'État". Thesis, Université de Lorraine, 2018. http://www.theses.fr/2018LORR0270.
Pełny tekst źródłaThe issue of jurisdictional immunity of states was for centuries an undisputed matter based on the principle of state equality and absolute independence of states. The rules were developed at a time when it was thought to be an infringement of a state's sovereignty to bring proceedings against it or its officials in a foreign country. However, the functions of states have changed over the centuries and nowadays states are involved in commercial activities as a private person and accordingly play an essential role in the commercial activities of the world. In fact, the issue of state immunities is an increasingly important and rapidly developing area of international law and practice. The state practice reflects the emerging global consensus that States and State enterprises can no longer claim absolute, unrestrained immunity from the proper jurisdiction of foreign courts, especially for their commercial activities. Therefore, although the law of state immunity is related to the grant of immunities to states to enable them to carry out their public functions effectively, modern international law does not require the courts of one state to refrain from deciding a case merely because a foreign state is an unwilling defendant. It is therefore important to know how a plea of state immunity may be made and to what type of dispute it applies
Alculumbre, Solana. "Division of Labor Between Distinct Human Plasmacytoid Dendritic Cell Subsets Following Viral Activation". Thesis, Université Paris-Saclay (ComUE), 2015. http://www.theses.fr/2015SACLS014.
Pełny tekst źródłaUnder microbial stimulation plasmacytoid pre-dendritic cells (pDC) secrete large amounts of type I interferon (IFN) and differentiate into mature dendritic cells capable of activating T cells. These innate and adaptive functions are thought to be induced sequentially in pDC through triggering of the IRF-7 and NFkB pathways, respectively. We found that viral activation of pDC induced their differentiation into three phenotypically distinct subsets: PD-L1+CD80- (P1), PD-L1+CD80+ (P2) and PD-L1-CD80+ (P3). P1 specifically produced IFN-α, indicating a specialization in innate immunity, while promoting weak activation and high IL-10 expression in CD4 T cells. Conversely, P3 showed increased expression of surface costimulatory molecules, improved migratory capacity, strong naïve CD4 T cell activation, and induction of Th2 differentiation. P2 had an intermediate functional profile. No conversion could be induced between subsets. We identified P1 in psoriatic skin, and blood from active lupus patients. Our results indicate reciprocal exclusion, rather than sequential link, of innate and adaptive pDC functions, with important implications in immune regulation and immunopathology
Zunino, Barbara. "Dialogue entre le métabolisme et l’immunité dans le traitement des cancers". Thesis, Nice, 2014. http://www.theses.fr/2014NICE4113.
Pełny tekst źródłaThe link between cell metabolism and cancer at the cellular level has long been known. Caloric restriction (CR) is known to prolong lifespan and to protect from cancer incidence. The molecular mechanisms involved in these benefic effects have been evaluated and may offer new opportunities for therapeutic intervention. Moreover, CR and CR-mimetics such as 2-deoxyglucose (2DG) has been shown to enhance chemotherapy efficiency and to induce an anti-cancer immune response. During the period of my PhD I demonstrated how the modulation of metabolism through caloric restriction or through its mimetics could significantly reduce the expression of the anti-apoptotic protein Mcl-1 and sensitize lymphoma-bearing mice to apoptosis induced by a Bcl-2/XL inhibitor, ABT-737. We have demonstrated that CR can control Mcl-1 translation and sensitize cells to ABT-737-induced death regardless of the presence or absence of p53 and/or of the main “BH3-only proteins”. Then, I focused on deciphering the molecular mechanisms allowing the Hyper-thermic Intra-Peritoneal Chemotherapy (HIPEC) to be beneficial to patients suffering from peritoneal carcinomatosis. Part of the protective effect was mediated through the induction of an efficient anti-cancer immune response. Next, I showed the involvement of heat shock proteins 90 (Hsp90) in the observed effect. Indeed, when Hsp90 was blocked we lost the protection induced by the HIPEC-treated cells, therefore underling the role of Hsp90 in this HIPEC-dependent induction of anti-cancer immune response
Champiat, Stéphane. "Caractérisation clinique et biologique de l’hyperprogression tumorale lors du blocage de la voie PD-1/PD-L1". Thesis, Université Paris-Saclay (ComUE), 2019. http://www.theses.fr/2019SACLS040.
Pełny tekst źródłaImmune checkpoint blocking antibodies are profoundly changing the management of patients with cancer. At the forefront of this novel anticancer agent class, anti-PD-1/PD-L1 antibodies can exhibit a significant activity by restoring an efficient antitumor T-cell response. As a result, these agents are now approved in various tumor types such as melanoma, squamous, and nonsquamous non–small cell lung cancer (NSCLC), renal cell carcinoma (RCC), head and neck squamous cell carcinoma (HNSCC) or bladder cancer. Interestingly, these new immunotherapies also result in novel tumor response patterns such as delayed tumor responses or pseudoprogressions. As experience grows with these therapeutics, anecdotal reports are relating rapid disease progressions, which could suggest that immune checkpoint blockade may have a deleterious effect by accelerating the disease in a subset of patients. This thesis work has made it possible to characterize clinically and biologically this phenomenon of accelerated tumor growth under anti-checkpoint immunotherapy, which we have defined as “hyperprogressive disease” (HPD). Transcriptomic analysis of tumour samples from these patients suggested a specific role for the myeloid environment
Yates, Philip John. "Immunity to paramyxoviruses". Thesis, Open University, 1995. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.262218.
Pełny tekst źródłaYang, Lili Rothenberg Ellen V. "Towards engineering immunity /". Diss., Pasadena, Calif. : California Institute of Technology, 2004. http://resolver.caltech.edu/CaltechETD:etd-06042004-000641.
Pełny tekst źródłaZunino, Barbara. "Dialogue entre le métabolisme et l’immunité dans le traitement des cancers". Electronic Thesis or Diss., Nice, 2014. http://www.theses.fr/2014NICE4113.
Pełny tekst źródłaThe link between cell metabolism and cancer at the cellular level has long been known. Caloric restriction (CR) is known to prolong lifespan and to protect from cancer incidence. The molecular mechanisms involved in these benefic effects have been evaluated and may offer new opportunities for therapeutic intervention. Moreover, CR and CR-mimetics such as 2-deoxyglucose (2DG) has been shown to enhance chemotherapy efficiency and to induce an anti-cancer immune response. During the period of my PhD I demonstrated how the modulation of metabolism through caloric restriction or through its mimetics could significantly reduce the expression of the anti-apoptotic protein Mcl-1 and sensitize lymphoma-bearing mice to apoptosis induced by a Bcl-2/XL inhibitor, ABT-737. We have demonstrated that CR can control Mcl-1 translation and sensitize cells to ABT-737-induced death regardless of the presence or absence of p53 and/or of the main “BH3-only proteins”. Then, I focused on deciphering the molecular mechanisms allowing the Hyper-thermic Intra-Peritoneal Chemotherapy (HIPEC) to be beneficial to patients suffering from peritoneal carcinomatosis. Part of the protective effect was mediated through the induction of an efficient anti-cancer immune response. Next, I showed the involvement of heat shock proteins 90 (Hsp90) in the observed effect. Indeed, when Hsp90 was blocked we lost the protection induced by the HIPEC-treated cells, therefore underling the role of Hsp90 in this HIPEC-dependent induction of anti-cancer immune response
Walker, Lee Charles. "Foreign State Immunity & Foreign Official Immunity: The Human Rights Dimension". Thesis, The University of Sydney, 2017. http://hdl.handle.net/2123/18198.
Pełny tekst źródłaTadie, Jean Marc. "Rôles clinico-biologiques du monoxyde d'azote produit par les voies aériennes". Thesis, Paris Est, 2010. http://www.theses.fr/2010PEST0053/document.
Pełny tekst źródłaIn the respiratory tract, NO is produced by a wide variety of cell types and is generated via oxidation of l-arginine that is catalyzed by the enzyme NO synthase (NOS). NOS exists in three distinct isoforms: neuronal NOS (NOS-1), inducible NOS (NOS-2), and endothelial NOS (NOS-3). NO derived from the constitutive isoforms of NOS (NOS-1 and NOS-3) and other NO-adduct molecules (nitrosothiols) have been shown to be modulators of bronchomotor tone. On the other hand, NO derived from NOS-2 seems to be a proinflammatory mediator with immunomodulatory effects. This thesis explores the physiological and pathophysiological role of endogenous nitric oxide in the airways, and the clinical aspects of monitoring nitric oxide in exhaled air of patients with respiratory disease.First Study: competition between nitric oxide synthases (NOSs) and arginases for their common substrate l-arginine could be involved in the regulation of cholinergic airway reactivity and subsequent airway remodeling. The aims of this study were to evaluate the relationships between the expression of this enzymatic balance and the effects of NOS and arginase inhibition on bronchoconstrictive response to acetylcholine of patients without and with early chronic obstructive pulmonary disease (COPD). Twenty-two human bronchi were investigated for immunohistochemistry and modulation of acetylcholine-induced airway constriction. Significantly increased expression of NOS2 in immunoblots of bronchial tissue and staining in smooth muscle cells was evidenced in patients with COPD compared with control subjects. Forced expiratory volume in 1 s (FEV1) and NOS2 expression were negatively correlated. Pharmacological experiments demonstrated that resting tension was elevated in COPD compared with control subjects and was positively correlated with the expression of NOS2. The sole effect of the specific arginase inhibitor Nomega-hydroxy-nor-L-arginine was to decrease sensitivity in COPD patients, whereas NG-nitro-L-arginine methyl ester unexpectedly decreased resting tension because of a non-cGMP-dependent effect. In conclusion, an upregulation of NOS2 expression in COPD patients is involved in airway tone regulation and functional airflow limitation, whereas increased arginase activity is involved in airway sensitivity.Second Study: the change in exhaled NO after cardio-pulmonary bypass remains controversial. The aims were to determine whether exhaled NO sources (alveolar or bronchial) are modified after bypass, and whether mechanical ventilation (MV) settings during bypass modify exhaled NO changes. Thirty-two patients were divided into three groups: without MV during bypass and positive end-expiratory pressure (PEEP) (n=12), dead space MV without PEEP (n=10) and dead space MV with PEEP (n=10). Alveolar NO concentration and bronchial NO flux were calculated before and 1h after surgery using a two-compartment model of NO exchange developed in spontaneous breathing patients. Whereas a significant decrease in bronchial NO was found after bypass in the two groups without PEEP during bypass, this decrease was not observed in patients with dead space ventilation with PEEP. Alveolar NO was not significantly modified whatever the ventilation settings. In conclusion, the impairment of bronchial NO seemed related to airway closure since dead space mechanical ventilation with PEEP prevented its decrease.Third Study: the development of biomarkers able to predict the occurrence of nosocomial infection could help manage preventive strategies, especially in medical patients whose degree of acquired immunosuppression may be variable. We hypothesized that the NO fraction present in the airways (upper and lower) of critically ill patients under mechanical ventilation could constitute such a biomarker. We conducted an observational study in a medical intensive care unit. Forty-five patients (26 men; 72 [25th-75th percentiles] years [56-82]; Simplified Acute Physiology Score II, 63 [50-81], 14 infected) under mechanical ventilation (>3 days) underwent on day 1 and day 3 of their stay: nasal and exhaled (partitioned in bronchial and alveolar sources) bedside NO measurements, determination of urine NO end products and plasma cytokine (IL-6, IL-10) concentrations, and Sequential Organ Failure Assessment score calculation. Nosocomial infection incidence was recorded during the 15 subsequent days. Fifteen patients (33%) acquired a nosocomial infection. Nasal NO was the only marker significantly different between patients with and without subsequent infection (day 1, 52 ppb [20-142] vs. 134 [84-203], P = 0.038; day 3, 98 ppb [22-140] vs. 225 [89-288], P = 0.006, respectively). Nasal NO fraction 148 ppb or less at day 3 had an 80% sensitivity, a 70% specificity, and an odds ratio of 2.7 (95% confidence interval, 1.9-3.8) to predict acquisition of nosocomial infection. Nasal NO seems to be a relatively sensitive and specific biomarker of subsequent nosocomial infection acquisition
Catozzi, Carlotta. "Water buffalo microbiota and immunity during infectious diseases". Doctoral thesis, Universitat Autònoma de Barcelona, 2020. http://hdl.handle.net/10803/670193.
Pełny tekst źródłaEl objetivo de la tesis es investigar la respuesta inmunitaria de los búfalos de agua (Bubalus bubalis) durante las enfermedades infecciosas (por ejemplo, mastitis, brucelosis y tuberculosis) y las enfermedades de producción, como las enfermedades metabólicas relacionadas con el periparto o el estrés. Debido a que el sistema inmunitario está relacionado con el entorno microbiano, también se ha caracterizado la composición de la microbiota de la leche. Hasta el momento, el sistema inmunitario del búfalo de agua no estaba bien caracterizado y la microbiota de la leche era desconocida. Aunque los búfalos sean sensibles a las mismas enfermedades que los rumiantes (como por ejemplo mastitis, tuberculosis, brucelosis), se desconoce el impacto de estas enfermedades en el sistema inmunitario de los búfalos. En comparación con los otros rumiantes, el búfalo de agua presenta diferencias anatómicas (por ejemplo, en la glándula mamaria y en la piel) y fisiológicas (enfermedades infecciosas y peripartos). Por lo tanto, es evidente que tanto el sistema inmune como la microbiota podrían presentar varias diferencias. En mi tesis doctoral, he abordado algunos de estos problemas. En primer lugar, se investigó la microbiota de leche de los búfalos de agua durante la enfermedad de la mastitis. En segundo lugar, se evaluó la respuesta inmunitaria en animales afectados por brucelosis y tuberculosis, mediante técnicas de expresión génica y miRNAs. Finalmente, se caracterizó el período de transición midiendo las proteínas de fase aguda para evaluar el estado de inflamación.
The thesis aims to investigate the immune response of water buffaloes (Bubalus bubalis) during infectious diseases (e.g. mastitis, brucellosis and tuberculosis) and productions diseases, such as peripartum related metabolic diseases or stress. Given the relationship between the microbial environment and the immune system, the microbiota content of milk has been identified as well. The immune system of water buffalo has been poorly addressed so far, not to mention the microbiota, which was unknown. Dairy water buffaloes are sensitive to the same diseases as dairy ruminants, such as for example mastitis, tuberculosis, brucellosis, but the impact of these diseases on water buffaloes’ immune system are unknown. Water buffalo presents anatomical (e.g. at mammary gland and skin level) and physiological (peripartum and infectious diseases) differences as compared to cow and other dairy ruminants. Therefore, it is evident that both the immune system and microbiota could present several differences. In my PhD thesis, I tried to address some of these issues. Firstly, the milk microbiota of water buffaloes was investigated in relation to mastitis disease. Secondly, the evaluation of the immune response, in terms of gene expression ad miRNAs, was carried out in animals affected by brucellosis and tuberculosis. Finally, the characterization of the transition period was performed measuring acute phase proteins to assess the inflammation status during the transition period.
Książki na temat "Immunity"
Immunity. New York: St. Martin's Minotaur, 2008.
Znajdź pełny tekst źródłaTotal immunity. London: Corvus, 2012.
Znajdź pełny tekst źródłaWeiner, Michael A. Maximum immunity. Boston: Houghton Mifflin, 1986.
Znajdź pełny tekst źródłaEzekowitz, R. Alan B., i Jules A. Hoffmann. Innate Immunity. New Jersey: Humana Press, 2002. http://dx.doi.org/10.1385/1592593208.
Pełny tekst źródłaSöderhäll, Kenneth, red. Invertebrate Immunity. Boston, MA: Springer US, 2010. http://dx.doi.org/10.1007/978-1-4419-8059-5.
Pełny tekst źródłaCullen, Bryan R., red. Intrinsic Immunity. Berlin, Heidelberg: Springer Berlin Heidelberg, 2013. http://dx.doi.org/10.1007/978-3-642-37765-5.
Pełny tekst źródłaPathak, J. P. N., red. Insect Immunity. Dordrecht: Springer Netherlands, 1993. http://dx.doi.org/10.1007/978-94-011-1618-3.
Pełny tekst źródłaEwbank, Jonathan, i Eric Vivier, red. Innate Immunity. Totowa, NJ: Humana Press, 2008. http://dx.doi.org/10.1007/978-1-59745-570-1.
Pełny tekst źródłaBona, Constantin, red. Neonatal Immunity. Totowa, NJ: Humana Press, 2005. http://dx.doi.org/10.1007/978-1-59259-825-0.
Pełny tekst źródłaNovaković, Marko, red. Diplomatic Immunity. Singapore: Springer Singapore, 2020. http://dx.doi.org/10.1007/978-981-15-1094-6.
Pełny tekst źródłaCzęści książek na temat "Immunity"
Wilson, Van G. "Immunity, Immunity, Immunity". W Viruses: Intimate Invaders, 95–119. Cham: Springer International Publishing, 2022. http://dx.doi.org/10.1007/978-3-030-85487-4_5.
Pełny tekst źródłaYakura, Hidetaka. "The Immune System at the Organism Level". W Immunity, 79–99. Boca Raton: CRC Press, 2024. http://dx.doi.org/10.1201/9781003486800-3.
Pełny tekst źródłaYakura, Hidetaka. "Autoimmunity, Symbiosis, and Organism". W Immunity, 43–78. Boca Raton: CRC Press, 2024. http://dx.doi.org/10.1201/9781003486800-2.
Pełny tekst źródłaYakura, Hidetaka. "The Immune System Omnipresent in the Biological World". W Immunity, 100–129. Boca Raton: CRC Press, 2024. http://dx.doi.org/10.1201/9781003486800-4.
Pełny tekst źródłaYakura, Hidetaka. "What Has Immunology Tried to Explain?" W Immunity, 1–42. Boca Raton: CRC Press, 2024. http://dx.doi.org/10.1201/9781003486800-1.
Pełny tekst źródłaYakura, Hidetaka. "Toward a New Philosophy of Life". W Immunity, 150–54. Boca Raton: CRC Press, 2024. http://dx.doi.org/10.1201/9781003486800-6.
Pełny tekst źródłaYakura, Hidetaka. "Metaphysics of Immunity". W Immunity, 130–49. Boca Raton: CRC Press, 2024. http://dx.doi.org/10.1201/9781003486800-5.
Pełny tekst źródłaHeppner, John B., D. G. Boucias, J. C. Pendland, Andrei Sourakov, Timothy Ebert, Roger Downer, Kun Yan Zhu i in. "Immunity". W Encyclopedia of Entomology, 1922–23. Dordrecht: Springer Netherlands, 2008. http://dx.doi.org/10.1007/978-1-4020-6359-6_1502.
Pełny tekst źródłaCutler, Gregg J. "Immunity". W Commercial Chicken Meat and Egg Production, 443–49. Boston, MA: Springer US, 2002. http://dx.doi.org/10.1007/978-1-4615-0811-3_24.
Pełny tekst źródłaBosch, Jos A. "Immunity". W Encyclopedia of Behavioral Medicine, 1149–50. Cham: Springer International Publishing, 2020. http://dx.doi.org/10.1007/978-3-030-39903-0_462.
Pełny tekst źródłaStreszczenia konferencji na temat "Immunity"
Hentley, William Thomas. "Bedbug cellular immunity". W 2016 International Congress of Entomology. Entomological Society of America, 2016. http://dx.doi.org/10.1603/ice.2016.109396.
Pełny tekst źródłaTimmis, Jon. "Engineering artificial immunity". W 2008 2nd IEEE International Conference on Digital Ecosystems and Technologies (DEST). IEEE, 2008. http://dx.doi.org/10.1109/dest.2008.4635098.
Pełny tekst źródłaIshida, Yoshiteru. "Immunity-based systems revisited". W the International Conference. New York, New York, USA: ACM Press, 2011. http://dx.doi.org/10.1145/2077489.2077538.
Pełny tekst źródłaDurier, Andre, Priscila Fernandez-Lopez, Jean-Luc Levant i Christian Marot. "ICIM-CPI: Integrated circuits immunity model: Conducted pulse immunity: Description, extraction and example". W 2018 IEEE International Symposium on Electromagnetic Compatibility and 2018 IEEE Asia-Pacific Symposium on Electromagnetic Compatibility (EMC/APEMC). IEEE, 2018. http://dx.doi.org/10.1109/isemc.2018.8393871.
Pełny tekst źródłaMaas, John. "Immunity to continuous RF disturbances". W 2008 IEEE International Symposium on Electromagnetic Compatibility - EMC 2008. IEEE, 2008. http://dx.doi.org/10.1109/isemc.2008.4652215.
Pełny tekst źródłaBraxton, Thomas E. "IEC transient-immunity testing overview". W 2008 IEEE International Symposium on Electromagnetic Compatibility - EMC 2008. IEEE, 2008. http://dx.doi.org/10.1109/isemc.2008.4652218.
Pełny tekst źródłaGiunta, G., i B. Audone. "Logistic Regression in Immunity Testing". W 2007 IEEE International Symposium on Electromagnetic Compatibility. IEEE, 2007. http://dx.doi.org/10.1109/isemc.2007.52.
Pełny tekst źródłaLawrence, Flynn. "The Future of immunity testing". W 2017 IEEE International Symposium on Electromagnetic Compatibility & Signal/Power Integrity (EMCSI). IEEE, 2017. http://dx.doi.org/10.1109/isemc.2017.8078003.
Pełny tekst źródłaMcGraw, Elizabeth A. "OnWolbachia, immunity and pathogen blocking". W 2016 International Congress of Entomology. Entomological Society of America, 2016. http://dx.doi.org/10.1603/ice.2016.94286.
Pełny tekst źródłaStanley, David W. "Eicosanoid signaling in insect immunity". W 2016 International Congress of Entomology. Entomological Society of America, 2016. http://dx.doi.org/10.1603/ice.2016.93559.
Pełny tekst źródłaRaporty organizacyjne na temat "Immunity"
Mukundan, Harshini. Agnostic Immunity [Slides]. Office of Scientific and Technical Information (OSTI), maj 2021. http://dx.doi.org/10.2172/1778724.
Pełny tekst źródłaIoannides, Constantin G. Tumor Immunity by Hydrophobic Bearing Antigens. Fort Belvoir, VA: Defense Technical Information Center, lipiec 2004. http://dx.doi.org/10.21236/ada436894.
Pełny tekst źródłaAndersen, Barbara L. Stress and Immunity Breast Cancer Project. Fort Belvoir, VA: Defense Technical Information Center, wrzesień 2001. http://dx.doi.org/10.21236/ada398948.
Pełny tekst źródłaAndersen, Barbara L. Stress and Immunity Breast Cancer Project. Fort Belvoir, VA: Defense Technical Information Center, wrzesień 1997. http://dx.doi.org/10.21236/ada334925.
Pełny tekst źródłaEck, Stephen, i Heike Boxhorn. Gene Therapy Mediated Breast Cancer Immunity. Fort Belvoir, VA: Defense Technical Information Center, wrzesień 1997. http://dx.doi.org/10.21236/ada335064.
Pełny tekst źródłaShrikant, Protul A. Epigenetic Regulation of Ovarian Tumor Immunity. Fort Belvoir, VA: Defense Technical Information Center, listopad 2010. http://dx.doi.org/10.21236/ada586321.
Pełny tekst źródłaShrikant, Protul A. Epigenetic Regulation of Ovarian Tumor Immunity. Fort Belvoir, VA: Defense Technical Information Center, listopad 2009. http://dx.doi.org/10.21236/ada589210.
Pełny tekst źródłaDisis, Mary L. Immunity to HER-1/neu Protein. Fort Belvoir, VA: Defense Technical Information Center, październik 1999. http://dx.doi.org/10.21236/ada390484.
Pełny tekst źródłaDisis, Mary L. Immunity to HER-1/neu Protein. Fort Belvoir, VA: Defense Technical Information Center, październik 2000. http://dx.doi.org/10.21236/ada391420.
Pełny tekst źródłaFrakes, Michael, i Jonathan Gruber. Defensive Medicine: Evidence from Military Immunity. Cambridge, MA: National Bureau of Economic Research, lipiec 2018. http://dx.doi.org/10.3386/w24846.
Pełny tekst źródła