Cytotoxic Activity of Dendritic Cells as a Possible Mechanism of Negative Regulation of T Lymphocytes in Pulmonary Tuberculosis

Сахно, Л. В.; Тихонова, М. А.; Тыринова, Т. В.; Леплина, О. Ю.; Shevela, Е. Ya.; Никонов, С. Д.; Жданов, О. А.; Ostanin, А. А.; Черных, Е. Р.

doi:10.1155/2012/628635

Cited by 14 publications

(12 citation statements)

References 24 publications

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“…The data obtained are consistent with those of Rajashree et al, which studied monocyte-derived DCs generated in presence of GM-CSF and IL-4 and found the inhibition of DC differentiation/maturation in pulmonary TB patients [18]. Besides, we for the first time have demonstrated that patient DCs had the increased expression of B7-H1 (PD-L1), known to induce T cell apoptosis and anergy upon interactions with PD-1 on T-cells [23]. The impairment of IFN-DC differentiation/activation in TB patients was associated with marked DCs dysfunction, in particular with altered cytokine production, decreased allostimulatory activity and the shift toward T2-stimulatory activity.…”

Section: Discussionsupporting

confidence: 91%

“…From this point of view, the prevalent T2-stimulating activity of IFN-DCs we have found in patients with active TB and especially in PPD-anergic patients, suggests that the DC alterations may be the cause of Th1 deficiency in pulmonary tuberculosis. Generally, the decreased allostimulatory activity, the dominance of T2 stimulating activity and the increased production of IL-10 along with our previous data on pro-apoptogenic activity of patient DCs [23], give evidence of "tolerogenic" phenotype of monocyte-derived DCs in TB infection. The engagement of PD-1/ PD-L1 (B7-H1) signaling pathway in DC cytotoxic activity was also demonstrated during tumor growth and in virus infections [28,30].…”

Section: Citationsupporting

confidence: 73%

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Low Antigen-specific T-cell Response in Pulmonary Tuberculosis is Associated with Impaired Phenotype and Functions of Interferon-α Induced Dendritic Cells

EYa¹

2013

J Clin Cell Immunol

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The phenotype and functions of monocyte-derived dendritic cells (DCs), generated upon stimulation with GM-CSF and IFN-α, were investigated in pulmonary tuberculosis (TB). The most pronounced increase of IL-10 production, as well as the decrease of allostimulatory activity and the alteration of T1/T2 stimulatory activity of DCs were registered in patients with low PPD-induced proliferative response. The data obtained evidence the tolerogenic phenotype of monocyte-derived IFN-DCs and the association of DC impairment with decreased antigen-specific T cell response in TB patients.

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Section: Discussionsupporting

confidence: 91%

Section: Citationsupporting

confidence: 73%

Low Antigen-specific T-cell Response in Pulmonary Tuberculosis is Associated with Impaired Phenotype and Functions of Interferon-α Induced Dendritic Cells

EYa¹

2013

J Clin Cell Immunol

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“…The ability of DCs to kill target cells that could serve in anti-tumor immunity or T-cell killing in autoimmunity and transplantation has been described (Chauvin and Josien, 2008). A recent study in pulmonary tuberculosis patients confirms the cytotoxic activity of DCs as a mechanism of negative regulation of T lymphocytes (Sakhno et al, 2012). In case of VD3-DCs, this action is antigen-dependent but not restricted to naïve T cells since VD3-DCs also block IFNγ and IL-10 production and induce active killing of a diabetogenic Th1 clone in an antigen-specific manner (van Halteren et al, 2002).…”

Section: Killing Of T Cells By Tolerogenic Dcs – the Story Of Mr Andmentioning

confidence: 77%

Regulatory Multitasking of Tolerogenic Dendritic Cells – Lessons Taken from Vitamin D3-Treated Tolerogenic Dendritic Cells

Nikolić¹,

Roep²

2013

Front. Immunol.

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Tolerogenic dendritic cells (DCs) work through silencing of differentiated antigen-specific T cells, activation and expansion of naturally occurring T regulatory cells (Tregs), transfer of regulatory properties to T cells, and the differentiation of naïve T cells into Tregs. Due to an operational definition based on T cell activation assays, the identity of tolerogenic DCs has been a matter of debate and it need not represent a specialized DC subset. Human tolerogenic DCs generated in vitro using inhibitory cytokines, growth factors, natural immunomodulators, or genetic manipulation have been effective and several of these tolerogenic DCs are currently being tested for clinical use. Ex vivo generated tolerogenic DCs reduce activation of naïve T cells using various means, promote a variety of regulatory T cells and most importantly, frequently show stable inhibitory phenotypes upon repetitive maturation with inflammatory factors. Yet, tolerogenic DCs differ with respect to the phenotype or the number of regulatory mechanisms they employ to modulate the immune system. In our experience, tolerogenic DCs generated using the biologically active form of vitamin D (VD3-DCs), alone, or combined with dexamethasone are proficient in their immunoregulatory functions. These tolerogenic DCs show a stable maturation-resistant semi-mature phenotype with low expression of activating co-stimulatory molecules, no production of the IL-12 family of cytokines and high expression of inhibitory molecules and IL-10. VD3-DCs induce increased apoptosis of effector T cells and induce antigen-specific regulatory T cells, which work through linked suppression ensuring infectious tolerance. Lessons learned on VD3-DCs help understanding the contribution of different pattern-recognition receptors (PRRs) and secondary signals to the tolerogenic function and how a cross-talk between DCs and T cells translates into immune regulation.

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“…Despite their seemingly preferential tumor-directed action, under certain circumstances, MoDCs can induce T cell death [21,32,37]. This observation was made in several studies ( Table 1); all of which were performed in the context of infectious diseases [21,32,37]. The first study demonstrated that MoDCs infected with measles virus can induce paracrine killing of autologous T cells [19].…”

Section: Killer Dcs In Humansmentioning

confidence: 99%

“…Conversely, another study found that CD40 ligation inhibits TRAIL expression in MoDCs, but the cytotoxic ability of these CD40L-matured MoDCs was preserved, suggesting TRAIL-independent mechanisms for induction of cell death [28]. Indeed, as outlined in Table 1, both cell contact-dependent and -independent mechanisms have been implicated in MoDC-mediated killing and their cytolytic armamentarium includes, in addition to TRAIL, a broad range of cytotoxic effector molecules such as TNFa [21][22][23][24]29,30], FAS-L [20][21][22]29,31,32], caspase-8 [19,[33][34][35], lymphotoxin (LT)-a1b2 [29], TNF-like weak inducer of apoptosis (TWEAK) [21], IFN-g [28], granzyme B [27,36], and programmed death ligand (PD-L1/2) [32,37].…”

Section: Killer Dcs In Humansmentioning

confidence: 99%

Tumoricidal activity of human dendritic cells

Tel

Anguille

Waterborg

et al. 2014

Trends in Immunology

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Dendritic cells (DCs) are a family of professional antigen-presenting cells (APCs) that are able to initiate innate and adaptive immune responses against pathogens and tumor cells. The DC family is heterogeneous and is classically divided into two main subsets, each with its unique phenotypic and functional characteristics: myeloid DCs (mDCs) and plasmacytoid DCs (pDCs). Recent results have provided intriguing evidence that both DC subsets can also function as direct cytotoxic effector cells; in particular, against cancer cells. In this review, we delve into this understudied function of human DCs and discuss why these so-called killer DCs might become important tools in future cancer immunotherapies.

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Cytotoxic Activity of Dendritic Cells as a Possible Mechanism of Negative Regulation of T Lymphocytes in Pulmonary Tuberculosis

Cited by 14 publications

References 24 publications

Low Antigen-specific T-cell Response in Pulmonary Tuberculosis is Associated with Impaired Phenotype and Functions of Interferon-α Induced Dendritic Cells

Low Antigen-specific T-cell Response in Pulmonary Tuberculosis is Associated with Impaired Phenotype and Functions of Interferon-α Induced Dendritic Cells

Regulatory Multitasking of Tolerogenic Dendritic Cells – Lessons Taken from Vitamin D3-Treated Tolerogenic Dendritic Cells

Tumoricidal activity of human dendritic cells

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