{"database":"biostudies-literature","file_versions":[],"scores":null,"additional":{"omics_type":["Unknown"],"volume":["21(1)"],"submitter":["Hayakawa K"],"pubmed_abstract":["Human old aged unmutated chronic lymphocytic leukemia U-CLL are the TCL1<sup>+</sup>ZAP70<sup>+</sup>CD5<sup>+</sup> B cells. Since CD5 makes the BCR signaling tolerance, ZAP70 increased in U-CLL not only TCL1<sup>+</sup> alone. In mice, TCL1 (TCL1A) is the negative from neonate to old aged, as TC<sup>-</sup>. V<sub>H</sub>8-12/V<sub>k</sub>21-5 is the anti-thymocyte/Thy-1 autoreactive ATA B cell. When ATA μκTg generation in mice, ATA B cells are the neonate generated CD5<sup>+</sup> B cells in B-1, and in the middle age, CD5<sup>+</sup> can be down or continuously CD5<sup>+</sup>, then, old aged CLL/lymphoma generation with increased CD11b in TC<sup>-</sup>ZAP70<sup>-</sup>CD5<sup>-</sup> or TC<sup>-</sup>ZAP70<sup>+</sup>CD5<sup>+</sup>. In this old aged TC<sup>-</sup>ATA B microarray analysis showed most similar to human CLL and U-CLL, and TC<sup>-</sup>ZAP70<sup>+</sup>CD5<sup>+</sup> showed certain higher present as U-CLL. Original neonate ATA B cells showed with several genes down or further increase in old aged tumor, and old aged T-bet<sup>+</sup>CD11c<sup>+</sup>, CTNNB1<sup>hi</sup>, HMGB<sup>hi</sup>, CXCR4<sup>hi</sup>, DPP4<sup>hi</sup> and decreased miR181b. These old aged increased genes and down miR181b are similar to human CLL. Also, in old age ATA B cell tumor, high CD38<sup>++</sup>CD44<sup>++</sup>, increased Ki67<sup>+</sup> AID<sup>+</sup>, and decreased CD180<sup>-</sup> miR15O<sup>low</sup> are similar to U-CLL. In this old aged ATA B, increased TLR7,9 and Wnt10b. TC<sup>+</sup>Tg generated with ATAμκTg mice occurred middle age tumor as TC<sup>+</sup>ZAP70<sup>-</sup>CD5<sup>+</sup> or TC<sup>+</sup>ZAP70<sup>+</sup>CD5<sup>+</sup>, with high NF-kB1, TLR4,6 and Wnt5b,6 without increased CD11b. Since neonatal state to age with TC<sup>+</sup>Tg continuously, middle age CLL/lymphoma generation is not similar to old aged generated, however, some increased in TC<sup>+</sup>ZAP70<sup>+</sup> are similar to the old age TC<sup>-</sup> ATA B tumor. Then, TC<sup>-</sup> ATA B old age tumor showed some difference to human CLL. ATA B cells showed CD11b<sup>+</sup>CD22<sup>++</sup>, CD24 down, and hepcidin Hamp2<sup>++</sup> with iron down. This mouse V8-12 similar to human V2-5, and V2-5 showed several cancers with macrophages/neutrophils generated hepcidin<sup>+</sup> iron<sup>low</sup> or some showed hepcidin<sup>-</sup> iron<sup>+</sup> with tumor, and mouse V8-12 with different V<sub>k</sub>19-17 generate MZ B cells strongly increased macrophage<sup>++</sup> in old aged and generated intestine/colon tumor. Conclusion, neonate generated TC<sup>-</sup>ATA B1 cells in old aged tumor generation are CD11b<sup>+</sup> in the leukemia CLL together with lymphoma cancer with hepcidin-related Hamp2<sup>++</sup> in B-1 cell generation to control iron."],"journal":["Immunity & ageing : I & A"],"pagination":["22"],"full_dataset_link":["https://www.ebi.ac.uk/biostudies/studies/S-EPMC10988983"],"repository":["biostudies-literature"],"pubmed_title":["B-1 derived anti-Thy-1 B cells in old aged mice develop lymphoma/leukemia with high expression of CD11b and Hamp2 that different from TCL1 transgenic mice."],"pmcid":["PMC10988983"],"pubmed_authors":["Shinton SA","Hayakawa K","Zhou Y"],"additional_accession":[]},"is_claimable":false,"name":"B-1 derived anti-Thy-1 B cells in old aged mice develop lymphoma/leukemia with high expression of CD11b and Hamp2 that different from TCL1 transgenic mice.","description":"Human old aged unmutated chronic lymphocytic leukemia U-CLL are the TCL1<sup>+</sup>ZAP70<sup>+</sup>CD5<sup>+</sup> B cells. Since CD5 makes the BCR signaling tolerance, ZAP70 increased in U-CLL not only TCL1<sup>+</sup> alone. In mice, TCL1 (TCL1A) is the negative from neonate to old aged, as TC<sup>-</sup>. V<sub>H</sub>8-12/V<sub>k</sub>21-5 is the anti-thymocyte/Thy-1 autoreactive ATA B cell. When ATA μκTg generation in mice, ATA B cells are the neonate generated CD5<sup>+</sup> B cells in B-1, and in the middle age, CD5<sup>+</sup> can be down or continuously CD5<sup>+</sup>, then, old aged CLL/lymphoma generation with increased CD11b in TC<sup>-</sup>ZAP70<sup>-</sup>CD5<sup>-</sup> or TC<sup>-</sup>ZAP70<sup>+</sup>CD5<sup>+</sup>. In this old aged TC<sup>-</sup>ATA B microarray analysis showed most similar to human CLL and U-CLL, and TC<sup>-</sup>ZAP70<sup>+</sup>CD5<sup>+</sup> showed certain higher present as U-CLL. Original neonate ATA B cells showed with several genes down or further increase in old aged tumor, and old aged T-bet<sup>+</sup>CD11c<sup>+</sup>, CTNNB1<sup>hi</sup>, HMGB<sup>hi</sup>, CXCR4<sup>hi</sup>, DPP4<sup>hi</sup> and decreased miR181b. These old aged increased genes and down miR181b are similar to human CLL. Also, in old age ATA B cell tumor, high CD38<sup>++</sup>CD44<sup>++</sup>, increased Ki67<sup>+</sup> AID<sup>+</sup>, and decreased CD180<sup>-</sup> miR15O<sup>low</sup> are similar to U-CLL. In this old aged ATA B, increased TLR7,9 and Wnt10b. TC<sup>+</sup>Tg generated with ATAμκTg mice occurred middle age tumor as TC<sup>+</sup>ZAP70<sup>-</sup>CD5<sup>+</sup> or TC<sup>+</sup>ZAP70<sup>+</sup>CD5<sup>+</sup>, with high NF-kB1, TLR4,6 and Wnt5b,6 without increased CD11b. Since neonatal state to age with TC<sup>+</sup>Tg continuously, middle age CLL/lymphoma generation is not similar to old aged generated, however, some increased in TC<sup>+</sup>ZAP70<sup>+</sup> are similar to the old age TC<sup>-</sup> ATA B tumor. Then, TC<sup>-</sup> ATA B old age tumor showed some difference to human CLL. ATA B cells showed CD11b<sup>+</sup>CD22<sup>++</sup>, CD24 down, and hepcidin Hamp2<sup>++</sup> with iron down. This mouse V8-12 similar to human V2-5, and V2-5 showed several cancers with macrophages/neutrophils generated hepcidin<sup>+</sup> iron<sup>low</sup> or some showed hepcidin<sup>-</sup> iron<sup>+</sup> with tumor, and mouse V8-12 with different V<sub>k</sub>19-17 generate MZ B cells strongly increased macrophage<sup>++</sup> in old aged and generated intestine/colon tumor. Conclusion, neonate generated TC<sup>-</sup>ATA B1 cells in old aged tumor generation are CD11b<sup>+</sup> in the leukemia CLL together with lymphoma cancer with hepcidin-related Hamp2<sup>++</sup> in B-1 cell generation to control iron.","dates":{"release":"2024-01-01T00:00:00Z","publication":"2024 Apr","modification":"2025-04-18T20:11:40.52Z","creation":"2025-04-07T08:06:17.419Z"},"accession":"S-EPMC10988983","cross_references":{"pubmed":["38570827"],"doi":["10.1186/s12979-024-00415-6"]}}