Anti–GM-CSF Autoantibodies in Patients with Cryptococcal Meningitis

Rosen, Lindsey B.; Freeman, Alexandra F.; Yang, Liyu; Jutivorakool, Kamonwan; Olivier, Kenneth N.; Angkasekwinai, Nasikarn; Suputtamongkol, Yupin; Bennett, John E.; Pyrgos, Vasilios; Williamson, Peter R.; Ding, Li; Holland, Steven M.; Browne, Sarah K.

doi:10.4049/jimmunol.1202526

Cited by 211 publications

(209 citation statements)

References 48 publications

(51 reference statements)

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“…Some of these disorders respond clinically to mechanism-based immunotherapy with IFN-γ or IFN-α (142). Similarly, neutralizing IFN-γ and GM-CSF autoantibodies can underlie adult-onset acquired immunodeficiency characterized by endemic dimorphic fungal (143) and CNS cryptococcal disease (144). Patients with alveolar proteinosis due to impaired GM-CSF signaling develop aspergillosis (145), consistent with murine studies (146).…”

Section: Antifungal Immunity: Lessons From Fungal Disease-associated supporting

confidence: 52%

Immunity against fungi

Lionakis¹,

Iliev²,

Hohl³

2017

JCI Insight

106

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Section: Antifungal Immunity: Lessons From Fungal Disease-associated supporting

confidence: 52%

Immunity against fungi

Lionakis¹,

Iliev²,

Hohl³

2017

JCI Insight

106

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“…7 (30, 31). As mentioned by Vella et al (30), the tumor Ag MUC-1 could also be the target of Abs in noncancer patients that could have been elicited by infection (56), as formally observed for GM-CSF autoantibodies (57). We cannot completely exclude a link between the anti-CCNB1 humoral response and the memory CCNB1-specific CD4 T cells that we detected in the short-term T cell assays, but there was no correlation between T and B cell responses.…”

Section: Discussioncontrasting

confidence: 37%

The Tumor Antigen Cyclin B1 Hosts Multiple CD4 T Cell Epitopes Differently Recognized by Pre-Existing Naive and Memory Cells in Both Healthy and Cancer Donors

Chevaleyre

Benhamouda

Favry

et al. 2015

The Journal of Immunology

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Cyclin B1 (CCNB1) is considered as a potential target for a cancer vaccine, as it is overexpressed in many malignant cells, while being transiently expressed in normal cells. To evaluate the CD4 T cell response to CCNB1, we derived T cell lines by multiple weekly rounds of stimulation with recombinant CCNB1 of T cells collected in healthy donors (long-term T cell assays). T cell lines were specific for 15 immunodominant peptides and derived preferentially from naive T cells. From 74 overlapping peptides, 20 peptides were selected for their broad specificity of binding to HLA class II molecules and included most of the immunodominant epitopes. They primed in vitro a large number of specific CD4 T cell lines in all the donors. Immunodominant epitopes were the most efficacious in long-term T cell assays, both in terms of number of specific T cell lines and number of responding donors. The 20 peptides were also submitted to short-term T cell assays using cells collected in healthy and cancer patients with the aim to evaluate the memory response. The recognized peptides differed from the immunodominant peptides and were part of the best promiscuous peptides. We also observed pre-existing CCNB1-specifc IgG Abs in both healthy and cancer donors. Long- and short-term T cell assays revealed that CCNB1 contained many CD4 T cell epitopes, which are differentially recognized by pre-existing naive and memory CD4 T cells. These observations are of value for the design of cancer vaccines.

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“…Patients with C. gattii infection may have subtle defects in immune function (276,279). Marr et al reported IgG2 antibody deficiency in one such patient (280).…”

Section: Epidemiology Of Human Infectionmentioning

confidence: 99%

“…In another PNG study, neither leukocyte antigen class I nor class II phenotypes were associated with C. gattii infection, although there was a trend toward increased susceptibility in patients carrying the human leukocyte antigen B*5601 (275). Recently, high levels of certain anticytokine antibodies (e.g., anti-granulocyte-macrophage colony-stimulating factor [GM-CSF] antibodies) were associated with cryptococcosis in HIV-negative patients (276). These antibodies predispose individuals to opportunistic infections by impairing innate immunity and may be especially relevant among HIV-negative patients in Asia (277,278).…”

Section: Epidemiology Of Human Infectionmentioning

confidence: 99%

Cryptococcus gattii Infections

2014

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SUMMARY Understanding of the taxonomy and phylogeny of Cryptococcus gattii has been advanced by modern molecular techniques. C. gattii probably diverged from Cryptococcus neoformans between 16 million and 160 million years ago, depending on the dating methods applied, and maintains diversity by recombining in nature. South America is the likely source of the virulent C. gattii VGII molecular types that have emerged in North America. C. gattii shares major virulence determinants with C. neoformans , although genomic and transcriptomic studies revealed that despite similar genomes, the VGIIa and VGIIb subtypes employ very different transcriptional circuits and manifest differences in virulence phenotypes. Preliminary evidence suggests that C. gattii VGII causes severe lung disease and death without dissemination, whereas C. neoformans disseminates readily to the central nervous system (CNS) and causes death from meningoencephalitis. Overall, currently available data indicate that the C. gattii VGI, VGII, and VGIII molecular types more commonly affect nonimmunocompromised hosts, in contrast to VGIV. New, rapid, cheap diagnostic tests and imaging modalities are assisting early diagnosis and enabling better outcomes of cerebral cryptococcosis. Complications of CNS infection include increased intracranial pressure, severe neurological sequelae, and development of immune reconstitution syndrome, although the mortality rate is low. C. gattii VGII isolates may exhibit higher fluconazole MICs than other genotypes. Optimal therapeutic regimens are yet to be determined; in most cases, initial therapy with amphotericin B and 5-flucytosine is recommended.

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Anti–GM-CSF Autoantibodies in Patients with Cryptococcal Meningitis

Cited by 211 publications

References 48 publications

Immunity against fungi

Immunity against fungi

The Tumor Antigen Cyclin B1 Hosts Multiple CD4 T Cell Epitopes Differently Recognized by Pre-Existing Naive and Memory Cells in Both Healthy and Cancer Donors

Cryptococcus gattii Infections

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