Unconventional T cells Flashcards

1
Q

Describe the main difference between group 1 and 2 CD1 proteins

A

Group 1 (CD1 A, B, C) are involved in the activation of T cell mediated responses. Group 2 (CD1 D) is involved in innate-like responses by priming iNKT responses.

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2
Q

What type of ligand is loaded and presented by CD1 proteins?

A

Glygolypids, with the sugar being the portion recognized by the TCR

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3
Q

Which conventional antigen-presenting molecule do CD1s resemble the most and why?

A

They are much more similar to MHC II. They present exogenous antigens, their expression is restricted to specific cell types, require lysosomal/endosomal acidification to present the peptide, have no requirement for TAP proteins to transport and load the peptide.

Similarities with MHC I: homodimer with beta2 microglobulin association

Unique feature: monomorphic.

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4
Q

What molecule increases the solubility of lipids in intracellular compartments?

A

MTP

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5
Q

Why is there a need for 5 different CD1s? Describe similarities and differences between the different CD1s

A

There is a need for 5 different CD1s because each of them loads lipids of different complexity given that they all migrate to different compartments in the endolysosomal pathway. They all have similar structures but the shape and size of the loading grooves differ between them.

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6
Q

Describe the process of self-potentiation mediated by group 1 CD1s

A

A DC gets infected (i.e. Mtb infection) and presents a pathogenic lipid on CD1s to a T cell=> T cell mediated cytotoxicity + secretion of antimicrobial mediators. The DC can simultaneously present endogenous self-lipids to an autoreactive T cell=> T cell mediated cytotoxicity + release of antimicrobial mediators (augmentation of the response).

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7
Q

How do you identify CD1 restricted T cells from a larger population?

A

Tetramers of CD1 molecules ligated to a fluorescently labelled molecule

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8
Q

Which CD1 molecules get preferentially recognized by alpha/beta and gamma/delta T cells?

A

ab=> CD1a

yd=> CD1c

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9
Q

Describe the role of CD1-restricted T cells in autoimmunity and regulation

A

self-lipids that stimulate a Th2 response lead to immunoregulation; self-lipids that stimulate a Th1/Th17 response lead to pathogenic T cells that can stimulate the production of autoantibodies.

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10
Q

How are immunostimulatory self lipids produced?

A

They can be produced from inhibitory self-lipids by the action of phospholipase enzymes (endogenous or exogenous)

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11
Q

How diverse/restricted is the TCR on innate-like lymphoid cells

A

The alpha chain is heavily restricted (AV1-2-AJ33 being the most common). The beta chain is also restricted to a relatively low number of recombination events, but it offers more diversity compared to the alpha chain (lecture 2, Dr. Salio, slide 5 on deep sequencing analysis).

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12
Q

Describe the key features of iNKT cells

A
Semi invariant TCR with identical CDR3a
Restricted by CD1d
Recognize glycolipids
Secrete IFN-y and IL-4 (Th1 vs Th2)
Can develop a memory-like phenotype
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13
Q

What is the most common ligand of iNKTs?

A

aGalCer

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14
Q

Describe the key features of MAIT cells

A

Semi invariant TCR
MR1-restricted
Mostly CD8+

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15
Q

Which ligands are immunostimulatory and immunoinhibitory for MAITs

A

Vitamin B2 derivatives are immunostimulatory

Vitamin B9 derivatives are immunoinhibitory

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16
Q

Describe the MR1 antigen presentation pathway

A

Resembles the MHC I pathway. Vitamin B2/9 can either be taken up by the surrounding environment or be produced by intracellular pathogens. They get loaded on MR1 expressed in the ER=> conformational change=> β€œOn” conformation=> secreted in vesicles to the cell surface.

17
Q

Briefly describe the development of iNKTs and MAITs

A

Both develop in the thymus by interacting with Haematopoietic cells. Microbial metabolites are also required for thymic MAITs development.
MAITs complete their development in the periphery; require interactions with microbial flora and B cells

18
Q

Describe different iNKT subsets.

A

type 1 iNKT=> low expression of PLZF (+ T-bet)
type 2=> high expression of PLZF (+ GATA3)
type 3=> intermediate expression of PLZF (+ RORyT)
Regulatory subset also recently descovered.

19
Q

Describe the main functions of iNKTs and MAITs

A

iNKTs: anti-microbial/viral; control incidence of diabetes, anti-tumoral.

MAITs: same as iNKT but seem to a poorer prognostic factor in tumour growth. They also have tissue repair potential.

20
Q

How are MAITs and iNKTs activated.

A

They can be activated both by immunostimulatory cytokines or by TCR/ pathogenic-ligand interactions.

21
Q

where are gamma-delta T cells localized?

A

They are localized to tissues

22
Q

Do gamma delta T cells migrate to LNs following maturation in the thymus

A

No

23
Q

Does the yd TCR have the potential to be more diverse compared to the conventional ab TCR? If so, how?

A

The yd TCR has the potential to be more diverse by incorporating an extra D segment while rearranging its delta chain.

24
Q

What determines the tissue a specific yd T cell will migrate to?

A

The variable gamma and delta segments that get rearranged and incorporated on the TCR determine the location of the yd T cell in the body

25
Q

Describe the roles of yd T cells

A

Response to microbial infections (HMBPP)
Response to tumor cells
Early immunoprotection in young animals
Immunoregulation, dampening of inflammation

26
Q

Describe the role of the hypervariable region 4 (HV4) in the yd TCR

A

It mediates the segregation of yd T cells to specific tissues by sensing tissue-specific antigens.l

27
Q

Do yd T cells recognize antigens in the context of MHC presentation?

A

No, the long CD1 and CD2 regions prevent interactions with MHC molecules.

28
Q

How do yd T cells sense foreign phosphoantigens?

A

The foreign phopshoantigens are released into a presenting cell (i.e. monocyte) and lead to the conformational change of butrophilin on the cell surface. The yd TCR is able to bind this altered butrophilin an d initiate a response.

29
Q

What ligands are recognized by yd T cells on stressed/cancer cells?

A

Unconventional MHC molecules:

MICA and MICB in humans
T10/22 in mice.

30
Q

Are yd T cells cytotoxic? If so, do they share the same mechanisms of killing employed by alpha/beta CTL?

A

They are cytotoxic and share the same mechanisms (Perforin+granzyme combo, FasL).