Natural killer cells might adapt their inhibitory receptors for memory | Vien Khoa Hoc Ky Thuat Nong Nghiep Mien Nam

Welcome To Website IAS

Home >> Updated News >> Natural killer cells might adapt their inhibitory receptors for memory

Hot news

Achievement

Independence Award

- First Rank - Second Rank - Third Rank

Labour Award

- First Rank - Second Rank -Third Rank

National Award

- Study on food stuff for animal(2005)

- Study on rice breeding for export and domestic consumption(2005)

VIFOTEC Award

- Hybrid Maize by Single Cross V2002 (2003)

- Tomato Grafting to Manage Ralstonia Disease(2005)

- Cassava variety KM140(2010)

Centres

Department of Biotechnology
https://sites.google.com/site/cadcnshias/
Dalat center
http://pvfcdalat.vn
Hung Loc Agricultural Research Center
http://harc-ias.vn/

Website links

Vietnamese calendar

Library

Visitors summary

Curently online : 14
Total visitors : 7455632

Updated News

Natural killer cells might adapt their inhibitory receptors for memory

Friday, 2018/11/09 | 08:12:32

Megan A. Cooper

PNAS November 6, 2018 115 (45) 11357-11359

Figure: Rag-deficient mice were sensitized with peptides by Wight et al. (1) to test NK cell antigen-specific recall responses in a model of CHS. While previous studies demonstrated strict specificity for antigens, these investigators found that peptides sharing the same amino acids at positions 2 and 3, thought to bind NK cell Ly49C, exhibited cross-reactivity.

Traditional teaching in immunology tells us that antigen-specific recall responses are the realm of adaptive immunity. However, over the past decade, there has been increasing evidence and interest in the concept of innate immune memory. Natural killer (NK) cells are the founding member of the innate lymphocyte family, initially recognized more than 40 y ago for their ability to kill tumor targets without prior sensitization across MHC haplotypes. Since that time, germline-encoded NK cell receptors (NKRs) that recognize class I MHC (MHC-I) molecules and deliver “activating” or “inhibitory” signals dictating NK cell education and function have been found. A decade ago, NK cells were discovered to have the capacity for specific recall responses to diverse antigens, akin to those seen in T cells. The mechanism by which NK cells specifically recognize a wide range of antigens is unknown. In PNAS, Wight et al. (1) provide evidence that inhibitory NKRs might recognize antigen in the context of MHC-I molecules to mediate NK cell memory responses.

The first evidence for NK cell memory responses came when O’Leary et al. (2) demonstrated that a subset of liver NK cells mediates hapten-specific contact hypersensitivity (CHS) in Rag-deficient mice. Adoptive transfer experiments of purified NK cells demonstrated specificity of long-lived NK cell recall responses (2, 3). Three major types of NK cell memory or memory-like responses are now recognized: antigen-specific responses, CMV-adapted memory (in the mouse reliant on a virally encoded ligand interacting with a germline-encoded NK cell-activating receptor), and cytokine-induced antigen-independent memory-like responses (2, 4 ⇓⇓–7). Wight et al. (1) focus on antigen-specific NK cell memory and investigate whether Ly49 inhibitory NKRs can recognize antigen.

Antigen-specific NK cell memory has been demonstrated for a wide variety of antigens, including haptens, viral-like particles, and in the context of infections such as influenza, vaccinia, and others (reviewed in ref. 7). Memory NK cell responses can be protective in vaccination models, and Paust et al. (3) showed that administration of inactivated vesicular stomatitis virus induced an NK cell population that conferred specific protection to lethal viral challenge in T and B cell-deficient mice. Prior sensitization with monobenzone enhanced NK cell antitumor responses to B16 melanoma tumor cells, thought to be due to monobenzone “haptenizing” melanocyte antigens (8). Although the concept of antigen-specific responses, independent of Rag-mediated receptor recombination, challenges the paradigms of immunological memory, results have been recapitulated in multiple independent studies in the mouse, and there is evidence of their existence in nonhuman primates and humans (7, 9). The mechanisms by which NK cells, which are not known to somatically rearrange receptors, can sense a wide array of antigens are unknown.

Wight et al. (1) used the CHS model to test whether inhibitory Ly49 NKRs are responsible for antigen recognition. In this model, haptens (small molecules that alter self-proteins) applied to the skin elicit specific recall responses in previously sensitized mice, measured as ear swelling and inflammatory infiltrate. While classically used to interrogate adaptive immunity, when done in Rag-deficient hosts lacking T and B cells, memory NK cell responses are detected (2). Wight et al. (1) used a genetic model in which Ly49 expression is severely reduced on a Rag1-deficient background to demonstrate that CHS to haptens and peptide antigens is not observed but can be rescued by transgenic expression of the inhibitory Ly49I receptor. Although suggestive of a requirement for Ly49 to recognize antigen, the model is complicated by the fact that in the absence of Ly49 receptors, NK cells are known to have poor function due to a lack of education (10). It was originally shown by O’Leary et al. (2) that NK cells with inhibitory Ly49 specific for self-MHC mediate CHS, which was thought to be related to an education requirement. Thus, it is difficult to distinguish the requirement for Ly49 for education versus memory response. Wight et al. (1) address this in two ways. First, they used F(ab′)₂ fragments of antibody to Ly49 receptors to inhibit Ly49 interactions without depleting cells. They blocked either Ly49C/I inhibitory receptors, which recognize MHC-I in C57BL/6 mice, or Ly49G inhibitory receptors, which do not have an MHC-I ligand in C57BL/6 mice. Results show that blocking inhibitory Ly49C/I, but not Ly49G, during either sensitization or challenge abrogated hapten-mediated CHS in Rag1-deficient mice. Second, they used MHC-I–deficient animals to demonstrate a lack of NK cell-mediated CHS, although this is again challenging since NK cells in this model are functionally deficient at baseline due to an education defect. However, they then tested MHC-I– or MCH-II–restricted ovalbumin peptides in a CHS model, demonstrating that antigen presented by MHC-I (which binds Ly49s), but not by MHC-II, can elicit an NK-mediated CHS response. Together, these results suggest that antigen presentation by relevant MHC-I and inhibitory Ly49 is required for NK cell antigen recall responses.

The authors hypothesize that because Ly49C binding has been reported to be sensitive to residues 2 and 3 of MHC-I antigen, there would be cross-reactivity of CHS responses to antigens with the same amino acids in these residues (1). Having demonstrated that peptides presented by MHC-I, but divergent at residues 2 and 3, elicit specific NK-mediated CHS responses without cross-reactivity, they tested a hybrid peptide that shares residues 2 and 3. Here, Wight et al. (1) observed cross-reactivity (i.e., mice sensitized with SIYNFEKL had a CHS response when challenged with SIYRYYGL, but not with SIINFEKL) (Fig. 1). Notably, this experiment is the first report of antigenic cross-reactivity in NK cell memory. These findings suggest that it may be possible to induce NK memory responses to a wide range of antigens by taking advantage of shared residues, although this will require additional testing. Lastly, they vaccinated Rag1-deficient mice with ovalbumin, followed by administering a melanoma tumor expressing ovalbumin protein. This vaccination strategy provided significant protection from tumor, consistent with prior studies using vaccination strategies targeting NK cells

See more: http://www.pnas.org/content/115/45/11357

Back

View: 412

[ Other News ]___________________________________________________