2016
DOI: 10.1182/blood-2016-04-712612
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CHAI and LATAIE: new genetic diseases of CTLA-4 checkpoint insufficiency

Abstract: CTLA-4 is a critical inhibitory “checkpoint” molecule of immune activation. Several recent reports have described patients with immune dysregulation and lymphoproliferative disease resulting from 2 different genetic diseases that directly or indirectly cause CTLA-4 deficiency. Numerous articles have also been published describing CTLA-4 blockade in cancer immunotherapy and its side effects, which are ultimately the consequence of treatment-induced CTLA-4 deficiency. Here, we review these 2 diseases and CTLA-4 … Show more

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Cited by 127 publications
(129 citation statements)
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“…However, in the absence of LRBA‐CTLA‐4 interaction (as seen in LRBA‐deficient patients), CTLA‐4‐containing vesicles are shuttled to lysosomes for degradation, thereby dampening the surface expression of CTLA‐4 4 . Impaired regulatory Treg functionality owing to the absence of LRBA might account for the development of autoimmune manifestations in LRBA‐deficient patients who are in fact similar to those reported in patients with heterozygous loss‐of‐function mutations in CTLA‐4 19 , 20 . However, the reduced CTLA‐4 expression does not explain the poor formation of memory B cells, and the defective production of specific antibodies (Abs) as reflected by the high frequency and recurrence of infections associated with LRBA deficiency 2 , 3 .…”
mentioning
confidence: 63%
“…However, in the absence of LRBA‐CTLA‐4 interaction (as seen in LRBA‐deficient patients), CTLA‐4‐containing vesicles are shuttled to lysosomes for degradation, thereby dampening the surface expression of CTLA‐4 4 . Impaired regulatory Treg functionality owing to the absence of LRBA might account for the development of autoimmune manifestations in LRBA‐deficient patients who are in fact similar to those reported in patients with heterozygous loss‐of‐function mutations in CTLA‐4 19 , 20 . However, the reduced CTLA‐4 expression does not explain the poor formation of memory B cells, and the defective production of specific antibodies (Abs) as reflected by the high frequency and recurrence of infections associated with LRBA deficiency 2 , 3 .…”
mentioning
confidence: 63%
“…LRBA deficiency leads to a secondary loss of CTLA‐4 protein and, consequently, defects in Treg function . LRBA has been found to bind the cytoplasmic tail of CTLA‐4 and protect it from degradation by blocking the trafficking of CTLA‐4 to lysosomes . This finding not only elucidated why the abundance of CTLA‐4 protein in LRBA patients was significantly lower than normal but also explained the overlap in clinical phenotype between CHAI and LATAIE patients .…”
Section: Lessons From the Treg Disordersmentioning
confidence: 87%
“…LRBA has been found to bind the cytoplasmic tail of CTLA‐4 and protect it from degradation by blocking the trafficking of CTLA‐4 to lysosomes . This finding not only elucidated why the abundance of CTLA‐4 protein in LRBA patients was significantly lower than normal but also explained the overlap in clinical phenotype between CHAI and LATAIE patients . Importantly, there is now extensive clinical experience using abatacept, which is a recombinant CTLA‐4 fusion protein drug, for the treatment of LATAIE, indicating its efficacy in ameliorating disease …”
Section: Lessons From the Treg Disordersmentioning
confidence: 95%
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