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Dissociating Siv Env And Cd4: Consequenes For Virus And Host
Dissociating Siv Env And Cd4: Consequenes For Virus And Host

... Swanstrom, Adrienne E., "Dissociating Siv Env and Cd4: Consequenes for Virus and Host" (2015). Publicly Accessible Penn ...
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... as cancers, autoimmune diseases and others. For instance, apoptotic cell death induction by chemotherapy in cancer is being applied to patients even though it has many weak points, such as the fact that apoptotic cells are usually ignored by the immune system since they are immunologically silent an ...
the innate immunity in bovine mastitis
the innate immunity in bovine mastitis

... The innate immune system represents the first line of defense in the host response to infection and is poised to immediately recognize and respond to the earliest stages of infection. The inherent capability of the innate system to respond to a vast number of pathogens is mediated by its ability to ...
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... significant portion of the emerging or re-emerging infectious diseases that are threatening our people and public health systems; moreover, many zoonotic pathogens are also known as “select agents,” which by definition could be used for bioterrorism or warfare. This illustrates the need for new, imp ...
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... Aerobic anoxygenic phototrophs also abundantly produce from one to over twenty different carotenoids per species (Fuchs et al. 2007; Yurkov and Beatty 1998), most of which are disengaged from photosynthetic energy transduction (Noguchi et al. 1992; Yurkov et al. 1993). Despite these features that di ...
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Complexity of complement activation in sepsis

... tissue damage. Therefore, complement can be currently viewed as an alarm system, which is capable of recognizing structures (danger-associated molecular patterns [DAMPs]) associated with a risk of the disturbance of homeostasis of either infectious or non-infectious origin. The classical pathway is ...
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Molecular mimicry

Molecular mimicry is defined as the theoretical possibility that sequence similarities between foreign and self-peptides are sufficient to result in the cross-activation of autoreactive T or B cells by pathogen-derived peptides. Despite the promiscuity of several peptide sequences which can be both foreign and self in nature, a single antibody or TCR (T cell receptor) can be activated by even a few crucial residues which stresses the importance of structural homology in the theory of molecular mimicry. Upon the activation of B or T cells, it is believed that these ""peptide mimic"" specific T or B cells can cross-react with self-epitopes, thus leading to tissue pathology (autoimmunity). Molecular mimicry is a phenomenon that has been just recently discovered as one of several ways in which autoimmunity can be evoked. A molecular mimicking event is, however, more than an epiphenomenon despite its low statistical probability of occurring and these events have serious implications in the onset of many human autoimmune disorders. In the past decade the study of autoimmunity, the failure to recognize self antigens as ""self,"" has grown immensely. Autoimmunity is a result of a loss of immunological tolerance, the ability for an individual to discriminate between self and non-self. Growth in the field of autoimmunity has resulted in more and more frequent diagnosis of autoimmune diseases. Consequently, recent data show that autoimmune diseases affect approximately 1 in 31 people within the general population. Growth has also led to a greater characterization of what autoimmunity is and how it can be studied and treated. With an increased amount of research, there has been tremendous growth in the study of the several different ways in which autoimmunity can occur, one of which is molecular mimicry. The mechanism by which pathogens have evolved, or obtained by chance, similar amino acid sequences or the homologous three-dimensional crystal structure of immunodominant epitopes remains a mystery.
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