Cargando…
The early intestinal immune response in experimental neonatal ovine cryptosporidiosis is characterized by an increased frequency of perforin expressing NCR1(+) NK cells and by NCR1(−) CD8(+) cell recruitment
Cryptosporidium parvum, a zoonotic protozoan parasite, causes important losses in neonatal ruminants. Innate immunity plays a key role in controlling the acute phase of this infection. The participation of NCR1+ Natural Killer (NK) cells in the early intestinal innate immune response to the parasite...
| Autores principales: | , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
BioMed Central
2015
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4355373/ https://www.ncbi.nlm.nih.gov/pubmed/25890354 http://dx.doi.org/10.1186/s13567-014-0136-1 |
| _version_ | 1782360845693485056 |
|---|---|
| author | Olsen, Line Åkesson, Caroline Piercey Storset, Anne K Lacroix-Lamandé, Sonia Boysen, Preben Metton, Coralie Connelley, Timothy Espenes, Arild Laurent, Fabrice Drouet, Françoise |
| author_facet | Olsen, Line Åkesson, Caroline Piercey Storset, Anne K Lacroix-Lamandé, Sonia Boysen, Preben Metton, Coralie Connelley, Timothy Espenes, Arild Laurent, Fabrice Drouet, Françoise |
| author_sort | Olsen, Line |
| collection | PubMed |
| description | Cryptosporidium parvum, a zoonotic protozoan parasite, causes important losses in neonatal ruminants. Innate immunity plays a key role in controlling the acute phase of this infection. The participation of NCR1+ Natural Killer (NK) cells in the early intestinal innate immune response to the parasite was investigated in neonatal lambs inoculated at birth. The observed increase in the lymphocyte infiltration was further studied by immunohistology and flow cytometry with focus on distribution, density, cellular phenotype related to cytotoxic function and activation status. The frequency of NCR1+ cells did not change with infection, while their absolute number slightly increased in the jejunum and the CD8+/NCR1- T cell density increased markedly. The frequency of perforin+ cells increased significantly with infection in the NCR1+ population (in both NCR1+/CD16+ and NCR1+/CD16- populations) but not in the NCR1-/CD8+ population. The proportion of NCR1+ cells co-expressing CD16+ also increased. The fraction of cells expressing IL2 receptor (CD25), higher in the NCR1+/CD8+ population than among the CD8+/NCR1- cells in jejunal Peyer’s patches, remained unchanged during infection. However, contrary to CD8+/NCR1- lymphocytes, the intensity of CD25 expressed by NCR1+ lymphocytes increased in infected lambs. Altogether, the data demonstrating that NK cells are highly activated and possess a high cytotoxic potential very early during infection, concomitant with an up-regulation of the interferon gamma gene in the gut segments, support the hypothesis that they are involved in the innate immune response against C. parvum. The early significant recruitment of CD8+/NCR1- T cells in the small intestine suggests that they could rapidly drive the establishment of the acquired immune response. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s13567-014-0136-1) contains supplementary material, which is available to authorized users. |
| format | Online Article Text |
| id | pubmed-4355373 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2015 |
| publisher | BioMed Central |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-43553732015-03-12 The early intestinal immune response in experimental neonatal ovine cryptosporidiosis is characterized by an increased frequency of perforin expressing NCR1(+) NK cells and by NCR1(−) CD8(+) cell recruitment Olsen, Line Åkesson, Caroline Piercey Storset, Anne K Lacroix-Lamandé, Sonia Boysen, Preben Metton, Coralie Connelley, Timothy Espenes, Arild Laurent, Fabrice Drouet, Françoise Vet Res Research Cryptosporidium parvum, a zoonotic protozoan parasite, causes important losses in neonatal ruminants. Innate immunity plays a key role in controlling the acute phase of this infection. The participation of NCR1+ Natural Killer (NK) cells in the early intestinal innate immune response to the parasite was investigated in neonatal lambs inoculated at birth. The observed increase in the lymphocyte infiltration was further studied by immunohistology and flow cytometry with focus on distribution, density, cellular phenotype related to cytotoxic function and activation status. The frequency of NCR1+ cells did not change with infection, while their absolute number slightly increased in the jejunum and the CD8+/NCR1- T cell density increased markedly. The frequency of perforin+ cells increased significantly with infection in the NCR1+ population (in both NCR1+/CD16+ and NCR1+/CD16- populations) but not in the NCR1-/CD8+ population. The proportion of NCR1+ cells co-expressing CD16+ also increased. The fraction of cells expressing IL2 receptor (CD25), higher in the NCR1+/CD8+ population than among the CD8+/NCR1- cells in jejunal Peyer’s patches, remained unchanged during infection. However, contrary to CD8+/NCR1- lymphocytes, the intensity of CD25 expressed by NCR1+ lymphocytes increased in infected lambs. Altogether, the data demonstrating that NK cells are highly activated and possess a high cytotoxic potential very early during infection, concomitant with an up-regulation of the interferon gamma gene in the gut segments, support the hypothesis that they are involved in the innate immune response against C. parvum. The early significant recruitment of CD8+/NCR1- T cells in the small intestine suggests that they could rapidly drive the establishment of the acquired immune response. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s13567-014-0136-1) contains supplementary material, which is available to authorized users. BioMed Central 2015-03-11 2015 /pmc/articles/PMC4355373/ /pubmed/25890354 http://dx.doi.org/10.1186/s13567-014-0136-1 Text en © Olsen et al.; licensee BioMed Central. 2015 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated. |
| spellingShingle | Research Olsen, Line Åkesson, Caroline Piercey Storset, Anne K Lacroix-Lamandé, Sonia Boysen, Preben Metton, Coralie Connelley, Timothy Espenes, Arild Laurent, Fabrice Drouet, Françoise The early intestinal immune response in experimental neonatal ovine cryptosporidiosis is characterized by an increased frequency of perforin expressing NCR1(+) NK cells and by NCR1(−) CD8(+) cell recruitment |
| title | The early intestinal immune response in experimental neonatal ovine cryptosporidiosis is characterized by an increased frequency of perforin expressing NCR1(+) NK cells and by NCR1(−) CD8(+) cell recruitment |
| title_full | The early intestinal immune response in experimental neonatal ovine cryptosporidiosis is characterized by an increased frequency of perforin expressing NCR1(+) NK cells and by NCR1(−) CD8(+) cell recruitment |
| title_fullStr | The early intestinal immune response in experimental neonatal ovine cryptosporidiosis is characterized by an increased frequency of perforin expressing NCR1(+) NK cells and by NCR1(−) CD8(+) cell recruitment |
| title_full_unstemmed | The early intestinal immune response in experimental neonatal ovine cryptosporidiosis is characterized by an increased frequency of perforin expressing NCR1(+) NK cells and by NCR1(−) CD8(+) cell recruitment |
| title_short | The early intestinal immune response in experimental neonatal ovine cryptosporidiosis is characterized by an increased frequency of perforin expressing NCR1(+) NK cells and by NCR1(−) CD8(+) cell recruitment |
| title_sort | early intestinal immune response in experimental neonatal ovine cryptosporidiosis is characterized by an increased frequency of perforin expressing ncr1(+) nk cells and by ncr1(−) cd8(+) cell recruitment |
| topic | Research |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4355373/ https://www.ncbi.nlm.nih.gov/pubmed/25890354 http://dx.doi.org/10.1186/s13567-014-0136-1 |
| work_keys_str_mv | AT olsenline theearlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT akessoncarolinepiercey theearlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT storsetannek theearlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT lacroixlamandesonia theearlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT boysenpreben theearlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT mettoncoralie theearlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT connelleytimothy theearlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT espenesarild theearlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT laurentfabrice theearlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT drouetfrancoise theearlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT olsenline earlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT akessoncarolinepiercey earlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT storsetannek earlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT lacroixlamandesonia earlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT boysenpreben earlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT mettoncoralie earlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT connelleytimothy earlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT espenesarild earlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT laurentfabrice earlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment AT drouetfrancoise earlyintestinalimmuneresponseinexperimentalneonatalovinecryptosporidiosisischaracterizedbyanincreasedfrequencyofperforinexpressingncr1nkcellsandbyncr1cd8cellrecruitment |