Immunological memory is the ability of the immune system to quickly and specifically recognize an antigen that the body has previously encountered and initiate a corresponding immune response. Generally, they are secondary, tertiary and other subsequent immune responses to the same antigen. The adaptive immune system and antigen-specific receptor generation (TCR, antibodies) are responsible for adaptive immune memory.[citation needed]
After the inflammatory immune response to danger-associated antigen, some of the antigen-specific T cells and B cells persist in the body and become long-living memory T and B cells. After the second encounter with the same antigen, they recognize the antigen and mount a faster and more robust response. Immunological memory is the basis of vaccination.[1][2] Emerging resources show that even the innate immune system can initiate a more efficient immune response and pathogen elimination after the previous stimulation with a pathogen, respectively with PAMPs or DAMPs. Innate immune memory (also called trained immunity) is neither antigen-specific nor dependent on gene rearrangement, but the different response is caused by changes in epigenetic programming and shifts in cellular metabolism. Innate immune memory was observed in invertebrates as well as in vertebrates.[3][4]
Adaptive immune memory
editDevelopment of adaptive immune memory
editImmunological memory occurs after a primary immune response against the antigen. Immunological memory is thus created by each individual, after a previous initial exposure, to a potentially dangerous agent. The course of secondary immune response is similar to primary immune response. After the memory B cell recognizes the antigen it presents the peptide: MHC II complex to nearby effector T cells. That leads to activation of these cells and rapid proliferation of cells. After the primary immune response has disappeared, the effector cells of the immune response are eliminated.[5]
However, antibodies that were previously created in the body remain and represent the humoral component of immunological memory and comprise an important defensive mechanism in subsequent infections. In addition to the formed antibodies in the body there remains a small number of memory T and B cells that make up the cellular component of the immunological memory. They stay in blood circulation in a resting state and at the subsequent encounter with the same antigen these cells are able to respond immediately and eliminate the antigen. Memory cells have a long life and last up to several decades in the body.[6][2]
Immunity to chickenpox, measles, and some other diseases lasts a lifetime. Immunity to many diseases eventually wears off. The immune system's response to a few diseases, such as dengue, counterproductively worsens the next infection (antibody-dependent enhancement).[7]
As of 2019, researchers are still trying to find out why some vaccines produce life-long immunity, while the effectiveness of other vaccines drops to zero in less than 30 years (for mumps) or less than six months (for H3N2 influenza).[8]
Evolution of adaptive immune memory
editThe evolutionary invention of memory T and B cells is widespread; however, the conditions required to develop this costly adaptation are specific. First, in order to evolve immune memory the initial molecular machinery cost must be high and will demand losses in other host characteristics. Second, middling or long lived organisms have higher chance of evolving such apparatus. The cost of this adaption increases if the host has a middling lifespan as the immune memory must be effective earlier in life.[9]
Furthermore, research models show that the environment plays an essential role in the diversity of memory cells in a population. Comparing the influence of multiple infections to a specific disease as opposed to disease diversity of an environment provide evidence that memory cell pools accrue diversity based on the number of individual pathogens exposed, even at the cost of efficiency when encountering more common pathogens. Individuals living in isolated environments such as islands have a less diverse population of memory cells, which are, however, present with sturdier immune responses. That indicates that the environment plays a large role in the evolution of memory cell populations.[10]
Previously acquired immune memory can be depleted by measles in unvaccinated children, leaving them at risk of infection by other pathogens in the years after infection.[11]
Memory B cells
editMemory B cells are plasma cells that are able to produce antibodies for a long time. Unlike the naive B cells involved in the primary immune response the memory B cell response is slightly different. The memory B cell has already undergone clonal expansion, differentiation and affinity maturation, so it is able to divide multiple times faster and produce antibodies with much higher affinity (especially IgG).[1]
In contrast, the naive plasma cell is fully differentiated and cannot be further stimulated by antigen to divide or increase antibody production. Memory B cell activity in secondary lymphatic organs is highest during the first 2 weeks after infection. Subsequently, after 2 to 4 weeks its response declines. After the germinal center reaction the memory plasma cells are located in the bone marrow which is the main site of antibody production within the immunological memory.[12]
Memory T cells
editMemory T cells can be both CD4+ and CD8+. These memory T cells do not require further antigen stimulation to proliferate; therefore, they do not need a signal via MHC.[13] Memory T cells can be divided into two functionally distinct groups based on the expression of the CCR7 chemokine receptor. This chemokine indicates the direction of migration into secondary lymphatic organs. Those memory T cells that do not express CCR7 (these are CCR7-) have receptors to migrate to the site of inflammation in the tissue and represent an immediate effector cell population. These cells were named memory effector T cells (TEM). After repeated stimulation they produce large amounts of IFN-γ, IL-4 and IL-5. In contrast, CCR7 + memory T cells lack proinflammatory and cytotoxic function but have receptors for lymph node migration. These cells were named central memory T cells (TCM). They effectively stimulate dendritic cells, and after repeated stimulation they are able to differentiate in CCR7- effector memory T cells. Both populations of these memory cells originate from naive T cells and remain in the body for several years after initial immunization.[14]
Experimental techniques used to study these cells include measuring antigen-stimulated cell proliferation and cytokine release, staining with peptide-MHC multimers or using an activation-induced marker (AIM) assay.[15]
Innate immune memory
editMany invertebrates such as species of fresh water snails, copepod crustaceans, and tapeworms have been observed activating innate immune memory to instigate a more efficient immune response to second encounter with specific pathogens, despite missing an adaptive branch of the immune system.[3] RAG1-deficient mice without functional T and B cells were able to survive the administration of a lethal dose of Candida albicans when exposed previously to a much smaller amount, showing that vertebrates also retain this ability.[4] Despite not having the ability to manufacture antibodies like the adaptive immune system, innate immune system has immune memory properties as well. Innate immune memory (trained immunity) is defined as a long-term functional reprogramming of innate immune cells evoked by exogenous or endogenous insults and leading to an altered response towards a second challenge after returning to a non-activated state.[16]
When innate immune cells receive an activation signal; for example, through recognition of PAMPs with PRRs, they start the expression of proinflammatory genes, initiate an inflammatory response, and undergo epigenetic reprogramming. After the second stimulation, the transcription activation is faster and more robust.[17] Immunological memory was reported in monocytes, macrophages, NK cells, ILC1, ILC2, and ILC3 cells.[18][17] Concomitantly, some nonimmune cells, for example, epithelial stem cells on barrier tissues, or fibroblasts, change their epigenetic state and respond differently after priming insult.[19]
Mechanism of innate immune memory
editAt the steady state, unstimulated cells have reduced biosynthetic activities and more condensed chromatin with reduced gene transcription. The interaction of exogenous PAMPs (β-glucan, muramyl peptide) or endogenous DAMPs (oxidized LDL, uric acid) with PRR initiates a cellular response. Triggered Intracellular signaling cascades lead to the upregulation of metabolic pathways such as glycolysis, Krebs cycle, and fatty acid metabolism. An increase in metabolic activity provides cells with energy and building blocks, which are needed for the production of signaling molecules such as cytokines and chemokines.[17]
Signal transduction changes the epigenetic marks and increases chromatin accessibility, to allow binding of transcription factors and start transcription of genes connected with inflammation. There is an interplay between metabolism and epigenetic changes because some metabolites such as fumarate and acetyl-CoA can activate or inhibit enzymes involved in chromatin remodeling.[16] After the stimulus let up, there is no need for immune factors production, and their expression in immune cells is terminated. Several epigenetic modifications created during stimulation remain. Characteristic epigenetic rewiring in trained cells is the accumulation of H3K4me3 on immune genes promoters and the increase of H3k4me1 and H3K27ac on enhancers. Additionally, cellular metabolism does not return to the state before stimulation, and trained cells remain in a prepared state. This status can last from weeks to several months and can be transmitted into daughter cells. Secondary stimulation induces a new response, which is faster and stronger.[16][17]
Evolution of innate immune memory
editImmune memory brings a major evolutionary advantage when the organism faces repeated infections. Inflammation is very costly, and increased effectivity of response accelerates pathogen elimination and prevents damage to the host's own tissue. Classical adaptive immune memory evolved in jawed vertebrates and in jawless fish (lamprey), which is approximately just 1% of living organisms. Some form of immune memory is, therefore, reported in other species. In plants and invertebrates, faster kinetics, increased magnitude of immune response and an improved survival rate can be seem after secondary infection encounters. Immune memory is common for the vast majority of biodiversity on earth.[20]
It has been proposed that immune memory in innate and adaptive immunity represents an evolutionary continuum in which a more robust immune response evolved first, mediated by epigenetic reprogramming. In contrast, specificity through antigen-specific receptors evolved later in some vertebrates.[21]
Evolutionary mechanisms leading to the development of immunological memory
editThe emergence of the adaptive immune system is rooted in the deep history of evolution dating back roughly 500 million years. Investigations and recent studies found that two major events led to the emergence of the same.[22] These two macroevolutionary events were the origin of RAG and two whole rounds of genome duplication (WGD).The early origins and evidence for emergence of features resembling AIS dates to the era where jawed and jawless vertebrates diverged phylogenetically. Early investigations around the 1970s led to the discovery of unique inverted repeat flanking signal sequences while groups studied the RAG genome.[23] These so-called RAG transposons invaded regions of genome which may have been involved in AIS. Culmination of several works and review suggests that these disruptions could have been selected for a rearrangement to maintain genomic integrity which ultimately led to mechanisms like RAG diversifications in AIS. This discovery led to the hypothesis that there was an invasion event of a regulatory element-like region because these repeats resembled a remnant transposable element.[24] This invasion was argued to be necessary for the emergence of BCR and TCR-dependent immunity as we see now in all gnathostomes .According to recent scientific findings around 450-500mya the vertebrate genome went through two rounds of whole genome duplication. This is usually referred to as the “2R hypothesis”. Such intense genomic events lead to gene sub-functionalization, neofunctionalization or in many cases lead to loss of functions. Ohno, 40 years ago proposed that the evolutionary events which led to whole genome duplication was key for the emergence of the diversity we see in adaptive immunity and memory.[25] Further works illustrate that newer genic regions which arose because of this duplication event, are major contributors to today's adaptive immune systems which control immunological memory in gnathostomes. Okada’s work on investigating ohnologues that arose from WGD is clear proof of the same, that today AIS systems are remnants of the WGD events
See also
editReferences
edit- ^ a b Murphy, Kenneth; Weaver, Casey (2017). Janeway's Immunology (9th ed.). New York & London: Garland Science. pp. 473–475. ISBN 9780815345510.
- ^ a b Hammarlund, Erika, et al. (2003). "Duration of antiviral immunity after smallpox vaccination." Nature medicine 9.9, 1131.
- ^ a b Crișan, Tania O.; Netea, Mihai G.; Joosten, Leo A. B. (April 2016). "Innate immune memory: Implications for host responses to damage-associated molecular patterns". European Journal of Immunology. 46 (4): 817–828. doi:10.1002/eji.201545497. ISSN 0014-2980. PMID 26970440.
- ^ a b Gourbal, Benjamin; Pinaud, Silvain; Beckers, Gerold J. M.; Van Der Meer, Jos W. M.; Conrath, Uwe; Netea, Mihai G. (2018-04-17). "Innate immune memory: An evolutionary perspective". Immunological Reviews. 283 (1): 21–40. doi:10.1111/imr.12647. ISSN 0105-2896. PMID 29664574. S2CID 4891922.
- ^ Sprent, Jonathan, and Susan R. Webb. "Intrathymic and extrathymic clonal deletion of T cells." Current opinion in immunology 7.2 (1995): 196-205.
- ^ Crotty, Shane, et al. "Cutting edge: long-term B cell memory in humans after smallpox vaccination." The Journal of Immunology 171.10 (2003): 4969-4973.
- ^ Ed Yong. "Immunology Is Where Intuition Goes to Die". 2020. quote: "Immunity lasts a lifetime for some diseases—chickenpox, measles—but eventually wears off for many others." quote: "For some diseases, like dengue, an antibody response to one infection can counterintuitively make the next infection more severe."
- ^ Jon Cohen. "How long do vaccines last?". 2019.
- ^ Best, Alex; Hoyle, Andy (2013-06-06). "The evolution of costly acquired immune memory". Ecology and Evolution. 3 (7): 2223–2232. Bibcode:2013EcoEv...3.2223B. doi:10.1002/ece3.611. ISSN 2045-7758. PMC 3728959. PMID 23919164.
- ^ Graw, Frederik; Magnus, Carsten; Regoes, Roland R (2010). "Theoretical analysis of the evolution of immune memory". BMC Evolutionary Biology. 10 (1): 380. Bibcode:2010BMCEE..10..380G. doi:10.1186/1471-2148-10-380. ISSN 1471-2148. PMC 3018457. PMID 21143840.
- ^ Mina MJ, Kula T, Leng Y, Li M, Vries RD, Knip M, et al. (2019-11-01). "Measles virus infection diminishes preexisting antibodies that offer protection from other pathogens". Science. 366 (6465): 599–606. Bibcode:2019Sci...366..599M. doi:10.1126/science.aay6485. hdl:10138/307628. ISSN 0036-8075. PMC 8590458. PMID 31672891. S2CID 207815213.
- ^ Slifka, Mark K., Mehrdad Matloubian, and Rafi Ahmed (1995). "Bone marrow is a major site of long-term antibody production after acute viral infection." Journal of Virology, 69(3), 1895–1902.
- ^ Kassiotis, George, et al. "Impairment of immunological memory in the absence of MHC despite survival of memory T cells." Nature immunology 3.3 (2002): 244.
- ^ Sallusto, Federica, et al. "Two subsets of memory T lymphocytes with distinct homing potentials and effector functions." Nature 401.6754 (1999): 708.
- ^ Poloni, Chad; Schonhofer, Cole; Ivison, Sabine; Levings, Megan K.; Steiner, Theodore S.; Cook, Laura (2023-02-24). "T-cell activation-induced marker assays in health and disease". Immunology and Cell Biology. 101 (6): 491–503. doi:10.1111/imcb.12636. ISSN 1440-1711. PMC 10952637. PMID 36825901.
- ^ a b c Netea, Mihai G.; Domínguez-Andrés, Jorge; Barreiro, Luis B.; Chavakis, Triantafyllos; Divangahi, Maziar; Fuchs, Elaine; Joosten, Leo A. B.; van der Meer, Jos W. M.; Mhlanga, Musa M.; Mulder, Willem J. M.; Riksen, Niels P.; Schlitzer, Andreas; Schultze, Joachim L.; Stabell Benn, Christine; Sun, Joseph C. (June 2020). "Defining trained immunity and its role in health and disease". Nature Reviews Immunology. 20 (6): 375–388. doi:10.1038/s41577-020-0285-6. ISSN 1474-1741. PMC 7186935. PMID 32132681.
- ^ a b c d Fanucchi, Stephanie; Domínguez-Andrés, Jorge; Joosten, Leo A. B.; Netea, Mihai G.; Mhlanga, Musa M. (2021-01-12). "The Intersection of Epigenetics and Metabolism in Trained Immunity". Immunity. 54 (1): 32–43. doi:10.1016/j.immuni.2020.10.011. hdl:2066/229964. ISSN 1074-7613. PMID 33220235. S2CID 227124221.
- ^ Hartung, Franziska; Esser-von Bieren, Julia (2022-09-05). "Trained immunity in type 2 immune responses". Mucosal Immunology. 15 (6): 1158–1169. doi:10.1038/s41385-022-00557-0. ISSN 1935-3456. PMC 9705254. PMID 36065058.
- ^ Ordovas-Montanes, Jose; Beyaz, Semir; Rakoff-Nahoum, Seth; Shalek, Alex K. (May 2020). "Distribution and storage of inflammatory memory in barrier tissues". Nature Reviews Immunology. 20 (5): 308–320. doi:10.1038/s41577-019-0263-z. ISSN 1474-1741. PMC 7547402. PMID 32015472.
- ^ Netea, Mihai G.; Schlitzer, Andreas; Placek, Katarzyna; Joosten, Leo A. B.; Schultze, Joachim L. (2019-01-09). "Innate and Adaptive Immune Memory: an Evolutionary Continuum in the Host's Response to Pathogens". Cell Host & Microbe. 25 (1): 13–26. doi:10.1016/j.chom.2018.12.006. ISSN 1931-3128. PMID 30629914. S2CID 58623144.
- ^ Divangahi, Maziar; Aaby, Peter; Khader, Shabaana Abdul; Barreiro, Luis B.; Bekkering, Siroon; Chavakis, Triantafyllos; van Crevel, Reinout; Curtis, Nigel; DiNardo, Andrew R.; Dominguez-Andres, Jorge; Duivenvoorden, Raphael; Fanucchi, Stephanie; Fayad, Zahi; Fuchs, Elaine; Hamon, Melanie (January 2021). "Trained immunity, tolerance, priming and differentiation: distinct immunological processes". Nature Immunology. 22 (1): 2–6. doi:10.1038/s41590-020-00845-6. ISSN 1529-2916. PMC 8020292. PMID 33293712.
- ^ Flajnik, Martin F.; Kasahara, Masanori (2010). "Origin and evolution of the adaptive immune system: Genetic events and selective pressures". Nature Reviews Genetics. 11: 47–59. doi:10.1038/nrg2703. PMC 3805090. PMID 19997068.
- ^ Flajnik, Martin F.; Kasahara, Masanori (2010). "Origin and evolution of the adaptive immune system: Genetic events and selective pressures". Nature Reviews Genetics. 11: 47–59. doi:10.1038/nrg2703. PMC 3805090. PMID 19997068.
- ^ Flajnik, Martin F.; Kasahara, Masanori (2010). "Origin and evolution of the adaptive immune system: Genetic events and selective pressures". Nature Reviews Genetics. 11: 47–59. doi:10.1038/nrg2703. PMC 3805090. PMID 19997068.
- ^ Flajnik, Martin F.; Kasahara, Masanori (2010). "Origin and evolution of the adaptive immune system: Genetic events and selective pressures". Nature Reviews Genetics. 11: 47–59. doi:10.1038/nrg2703. PMC 3805090.