Cargando…
CCL22 mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk
Chronic lymphoproliferative disorder of natural killer cells (CLPD-NK) is characterized by clonal expansion of NK cells where the underlying genetic mechanisms are incompletely understood. Here, we report somatic mutations in the chemokine gene CCL22 as the hallmark of a distinct subset of CLPD-NK....
| Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
2022
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9117519/ https://www.ncbi.nlm.nih.gov/pubmed/35513723 http://dx.doi.org/10.1038/s41588-022-01059-2 |
| _version_ | 1784710329130811392 |
|---|---|
| author | Baer, Constance Kimura, Shunsuke Rana, Mitra S. Kleist, Andrew B. Flerlage, Tim Feith, David J. Chockley, Peter Walter, Wencke Meggendorfer, Manja Olson, Thomas L. Cheon, HeeJin Olson, Kristine C. Ratan, Aakrosh Mueller, Martha-Lena Foran, James M. Janke, Laura J. Qu, Chunxu Porter, Shaina N. Pruett-Miller, Shondra M. Kalathur, Ravi C. Haferlach, Claudia Kern, Wolfgang Paietta, Elisabeth Thomas, Paul G. Babu, M. Madan Loughran, Thomas P. Iacobucci, Ilaria Haferlach, Torsten Mullighan, Charles G |
| author_facet | Baer, Constance Kimura, Shunsuke Rana, Mitra S. Kleist, Andrew B. Flerlage, Tim Feith, David J. Chockley, Peter Walter, Wencke Meggendorfer, Manja Olson, Thomas L. Cheon, HeeJin Olson, Kristine C. Ratan, Aakrosh Mueller, Martha-Lena Foran, James M. Janke, Laura J. Qu, Chunxu Porter, Shaina N. Pruett-Miller, Shondra M. Kalathur, Ravi C. Haferlach, Claudia Kern, Wolfgang Paietta, Elisabeth Thomas, Paul G. Babu, M. Madan Loughran, Thomas P. Iacobucci, Ilaria Haferlach, Torsten Mullighan, Charles G |
| author_sort | Baer, Constance |
| collection | PubMed |
| description | Chronic lymphoproliferative disorder of natural killer cells (CLPD-NK) is characterized by clonal expansion of NK cells where the underlying genetic mechanisms are incompletely understood. Here, we report somatic mutations in the chemokine gene CCL22 as the hallmark of a distinct subset of CLPD-NK. CCL22 mutations were enriched at highly conserved residues, were mutually exclusive of STAT3 mutations, and were associated with gene expression programs that resembled normal CD16(dim)/CD56(bright) NK cells. Mechanistically, the mutations resulted in ligand-biased chemokine receptor signaling, with decreased internalization of the G-protein-coupled receptor for CCL22, CCR4, via impaired β-arrestin recruitment. This resulted in increased cell chemotaxis in vitro, bidirectional crosstalk with the hematopoietic microenvironment, and enhanced NK cell proliferation in vivo in transgenic human IL-15 mice. Somatic CCL22 mutations illustrate a unique mechanism of tumor formation in which gain-of-function chemokine mutations promote tumorigenesis by biased G-protein-coupled receptor signaling and dysregulation of microenvironmental crosstalk. |
| format | Online Article Text |
| id | pubmed-9117519 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2022 |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-91175192022-11-05 CCL22 mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk Baer, Constance Kimura, Shunsuke Rana, Mitra S. Kleist, Andrew B. Flerlage, Tim Feith, David J. Chockley, Peter Walter, Wencke Meggendorfer, Manja Olson, Thomas L. Cheon, HeeJin Olson, Kristine C. Ratan, Aakrosh Mueller, Martha-Lena Foran, James M. Janke, Laura J. Qu, Chunxu Porter, Shaina N. Pruett-Miller, Shondra M. Kalathur, Ravi C. Haferlach, Claudia Kern, Wolfgang Paietta, Elisabeth Thomas, Paul G. Babu, M. Madan Loughran, Thomas P. Iacobucci, Ilaria Haferlach, Torsten Mullighan, Charles G Nat Genet Article Chronic lymphoproliferative disorder of natural killer cells (CLPD-NK) is characterized by clonal expansion of NK cells where the underlying genetic mechanisms are incompletely understood. Here, we report somatic mutations in the chemokine gene CCL22 as the hallmark of a distinct subset of CLPD-NK. CCL22 mutations were enriched at highly conserved residues, were mutually exclusive of STAT3 mutations, and were associated with gene expression programs that resembled normal CD16(dim)/CD56(bright) NK cells. Mechanistically, the mutations resulted in ligand-biased chemokine receptor signaling, with decreased internalization of the G-protein-coupled receptor for CCL22, CCR4, via impaired β-arrestin recruitment. This resulted in increased cell chemotaxis in vitro, bidirectional crosstalk with the hematopoietic microenvironment, and enhanced NK cell proliferation in vivo in transgenic human IL-15 mice. Somatic CCL22 mutations illustrate a unique mechanism of tumor formation in which gain-of-function chemokine mutations promote tumorigenesis by biased G-protein-coupled receptor signaling and dysregulation of microenvironmental crosstalk. 2022-05 2022-05-05 /pmc/articles/PMC9117519/ /pubmed/35513723 http://dx.doi.org/10.1038/s41588-022-01059-2 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: https://www.springernature.com/gp/open-research/policies/accepted-manuscript-terms |
| spellingShingle | Article Baer, Constance Kimura, Shunsuke Rana, Mitra S. Kleist, Andrew B. Flerlage, Tim Feith, David J. Chockley, Peter Walter, Wencke Meggendorfer, Manja Olson, Thomas L. Cheon, HeeJin Olson, Kristine C. Ratan, Aakrosh Mueller, Martha-Lena Foran, James M. Janke, Laura J. Qu, Chunxu Porter, Shaina N. Pruett-Miller, Shondra M. Kalathur, Ravi C. Haferlach, Claudia Kern, Wolfgang Paietta, Elisabeth Thomas, Paul G. Babu, M. Madan Loughran, Thomas P. Iacobucci, Ilaria Haferlach, Torsten Mullighan, Charles G CCL22 mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk |
| title | CCL22 mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk |
| title_full | CCL22 mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk |
| title_fullStr | CCL22 mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk |
| title_full_unstemmed | CCL22 mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk |
| title_short | CCL22 mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk |
| title_sort | ccl22 mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk |
| topic | Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9117519/ https://www.ncbi.nlm.nih.gov/pubmed/35513723 http://dx.doi.org/10.1038/s41588-022-01059-2 |
| work_keys_str_mv | AT baerconstance ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT kimurashunsuke ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT ranamitras ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT kleistandrewb ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT flerlagetim ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT feithdavidj ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT chockleypeter ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT walterwencke ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT meggendorfermanja ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT olsonthomasl ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT cheonheejin ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT olsonkristinec ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT ratanaakrosh ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT muellermarthalena ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT foranjamesm ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT jankelauraj ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT quchunxu ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT portershainan ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT pruettmillershondram ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT kalathurravic ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT haferlachclaudia ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT kernwolfgang ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT paiettaelisabeth ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT thomaspaulg ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT babummadan ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT loughranthomasp ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT iacobucciilaria ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT haferlachtorsten ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk AT mullighancharlesg ccl22mutationsdrivenaturalkillercelllymphoproliferativediseasebyderegulatingmicroenvironmentalcrosstalk |