Systemic Human ILC Precursors Provide a Substrate for Tissue ILC Differentiation

Lim, Ai Ing; Li, Yan; López-Lastra, Silvia; Stadhouders, Ralph; Paul, Franziska; Casrouge, Armanda; Serafini, Nicolas; Puel, Anne; Bustamante, Jacinta; Surace, Laura; Masse‐Ranson, Guillemette; David, Eyal; Strick‐Marchand, Hélène; Bourhis, Lionel Le; Cocchi, R; Topazio, Davide; Graziano, Paolo; Muscarella, Lucia Anna; Rogge, Lars; Norel, Xavier; Sallenave, Jean–Michel; Allez, Matthieu; Graf, Thomas; Hendriks, Rudolf W.; Casanova, Jean‐Laurent; Amit, Ido; Yssel, Hans; Santo, James P. Di

doi:10.1016/j.cell.2017.02.021

Cited by 417 publications

(636 citation statements)

References 52 publications

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“…Murine parabiosis experiments showed that in adults ~95% of ILC2s do not apparently circulate in blood or replenish from blood-borne precursors, although small numbers of ILC precursors were noted in blood (43). Similarly, rare ILC precursors and ILC2s were identified in human blood (62). Most tissue ILC2s are thought to arise from precursors seeded into tissues before birth, and there is a rapid rise of mature ILC2s in lungs and small intestine in the first weeks after birth (39, 44, 45).…”

Section: Discussionmentioning

confidence: 95%

A Major Population of Functional KLRG1– ILC2s in Female Lungs Contributes to a Sex Bias in ILC2 Numbers

et al. 2018

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Humans show significant sex differences in the incidence and severity of respiratory diseases, including asthma and virus infection. Sex hormones contribute to the female sex bias in type 2 inflammation associated with respiratory diseases, consistent with recent reports that female lungs harbor greater numbers of GATA-3–dependent group 2 innate lymphoid cells (ILC2s). In this study, we determined whether sex hormone levels govern sex differences in the numbers, phenotype, and function of ILC2s in the murine lung and bone marrow (BM). Our data show that lungs of female mice harbor significantly greater ILC2 numbers in homeostasis, in part due to a major subset of ILC2s lacking killer-cell lectin like receptor G1 (KLRG1), a population largely absent in male lungs. The KLRG1− ILC2s were capable of type 2 cytokine production and increased with age after sexual maturity, suggesting that a unique functional subset exists in females. Experiments with gonadectomized mice or mice bearing either global or lymphocyte restricted estrogen receptor α (Esr1) deficiency showed that androgens rather than estrogens regulated numbers of the KLRG1− ILC2 subset and ILC2 functional capacity in the lung and BM, as well as levels of GATA-3 expression in BM ILC2s. Furthermore, the frequency of BM PLZF+ ILC precursors was higher in males and increased by excess androgens, suggesting that androgens act to inhibit the transition of ILC precursors to ILC2s. Taken together, these data show that a functional subset of KLRG1− ILC2s in females contributes to the sex bias in lung ILC2s that is observed after reproductive age.

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Section: Discussionmentioning

confidence: 95%

A Major Population of Functional KLRG1– ILC2s in Female Lungs Contributes to a Sex Bias in ILC2 Numbers

et al. 2018

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“…33 However, we demonstrate that human NKp44 1 bona fide ILC3s from secondary lymphoid tissues can develop into functional equivalents of NK cells, and this developmental pathway, which demonstrates many similarities to NK-cell differentiation from stage 3 precursors, 17,18 might provide cytotoxic protection at mucosal barriers.…”

Section: Nkp44mentioning

confidence: 99%

Interleukins 12 and 15 induce cytotoxicity and early NK-cell differentiation in type 3 innate lymphoid cells

et al. 2017

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“…Toutefois, il semblerait que chez l'adulte, des précurseurs périphériques existent. En effet, des précurseurs de cellules NK ont été trouvés en dehors de la moelle osseuse chez l'homme comme chez la souris [30] et des précurseurs des ILC3 ont été identifiés dans les amygdales et le sang périphérique [57] chez l'homme [31]. Le rôle des CHILP de la moelle osseuse chez l'adulte reste à définir.…”

Section: Transition Ilc1-ilc2unclassified

Les cellules lymphoïdes innées

et al. 2017

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Systemic Human ILC Precursors Provide a Substrate for Tissue ILC Differentiation

Cited by 417 publications

References 52 publications

A Major Population of Functional KLRG1– ILC2s in Female Lungs Contributes to a Sex Bias in ILC2 Numbers

A Major Population of Functional KLRG1– ILC2s in Female Lungs Contributes to a Sex Bias in ILC2 Numbers

Interleukins 12 and 15 induce cytotoxicity and early NK-cell differentiation in type 3 innate lymphoid cells

Les cellules lymphoïdes innées

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