Disseminated &lt;i&gt;Mycobacterium avium&lt;/i&gt; Infection in a 20-Year-Old Female with Partial Recessive IFNγR1 Deficiency

Remiszewski, P; Roszkowska-Sliz, Barbara; Winek, Jolanta; Chapgier, Ariane; Feinberg, Jeanne; Langfort, Renata; Bestry, Iwona; Augustynowicz–Kopeć, Ewa; Ptak, Jakub; Casanova, Jean‐Laurent; Rowińska-Zakrzewska, E

doi:10.1159/000088682

Cited by 46 publications

(31 citation statements)

References 31 publications

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“…1,2 Furthermore, humans with a disruption of the IFN-c signalling pathway show abnormal susceptibility to mycobacteria, 3 a condition that is reversed by the administration of synthetic IFN-c. 4 The central role of IFN-c means that most novel TB vaccine strategies have focused on generating strong T helper type 1 (Th1) responses either by using strong, Th1-polarizing adjuvants 5,6 or by heterologous prime-boost approaches. 7 The relevance of Th1 priming by these vaccines is indisputable and is supported by challenge studies involving experimental vaccines that induce different levels of IFN-c. 8 With the first novel vaccines now entering clinical trials, IFN-c has emerged as a surrogate marker for the protection conferred by the trial vaccine.…”

Section: Introductionmentioning

confidence: 99%

Adjuvant modulation of the cytokine balance in Mycobacterium tuberculosis subunit vaccines; immunity, pathology and protection

et al. 2008

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SummaryIt is known that protection against tuberculosis is mediated primarily by T helper type 1 (Th1) cells but the influence of the Th1/Th2 balance of a vaccination response on the subsequent protection and pathology during infection has not been studied in detail. We designed a panel of Ag85B-ESAT-6 subunit vaccines based on adjuvants with different Th1/Th2-promoting activities and studied cellular responses, bacterial replication and pathology in the lungs of mice infected with Mycobacterium tuberculosis. All vaccines induced cell-mediated and humoral responses but with markedly different interferon-c : interleukin-5 (IFN-c : IL-5) and immunoglobulin G1 (IgG1) : IgG2 ratios. The vaccines promoted different levels of control of bacterial replication with the most efficient protection being exerted by cationic liposomes containing monophosphoryl lipid A and low to completely absent immunity with conventional aluminium. The level of protection correlated with the amount of IFN-c produced in response to the vaccine whereas there was no inverse correlation with the level of IL-5. Characterizing a protective response was an accelerated recruitment of IL-17 and IFN-c-producing lymphocytes resulting in the early formation of granulomas containing clustered inducible nitric oxide synthase-activated macrophages. In comparison, non-protected mice exhibited a different inflammatory infiltrate rich in neutrophil granulocytes. This study indicates that the adjuvant component of a tuberculosis vaccine may be crucial in determining the kinetics by which effective granulomas, pivotal in controlling bacterial growth, are formed.

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Section: Introductionmentioning

confidence: 99%

Adjuvant modulation of the cytokine balance in Mycobacterium tuberculosis subunit vaccines; immunity, pathology and protection

et al. 2008

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“…30 Recessive complete IFNGR2 defi ciency can result in absence of IFNGR2 expression 30 or non-functional IFNGR2, 76,77 whereas the fi ve reported patients with recessive partial IFNGR2 defi ciency had normal to slightly lower IFNGR2 expression and residual interferon γ responses. 33,38,39 IFNGR2 haploinsuffi ciency can also confer dominant partial IFNGR2 defi ciency, 41 as can dominant negative mutations. 42 Generally, recessive com plete mutations result in more severe disease than partial defi ciencies.…”

Section: Il12 P40 Il12p35mentioning

confidence: 99%

“…42 Generally, recessive com plete mutations result in more severe disease than partial defi ciencies. 30,38,42,76 Flow cytometry can be used to detect surface IFNGR1 on peripheral blood mononuclear cells.…”

Section: Il12 P40 Il12p35mentioning

confidence: 99%

“…11,47,78,79 IFNGR2 expression is low and might need Epstein-Barr virus-transformed B cells to improve detection. 11,33 Some rare instances of patients with recessive complete IFNGR2 defi ciency and recessive partial IFNGR1 or IFNGR2 defi ciencies who have normal surface expression of hypofunctional receptors exist, 32,34,38,76 suggesting that genetic sequencing, a test for IFNGR function, or both must be used to confi rm the diagnosis. …”

Section: Il12 P40 Il12p35mentioning

confidence: 99%

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Host susceptibility to non-tuberculous mycobacterial infections

Holland

2015

The Lancet Infectious Diseases

202

175

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Non-tuberculous mycobacteria cause a broad range of clinical disorders, from cutaneous infections, such as cervical or intrathoracic lymphadenitis in children, to disseminated infections at all ages. Recognition of the underlying immune defect is crucial for rational treatment, preventive care, family screening, and, in some cases, transplantation. So far, at least seven autosomal mutations (in IL12B, IL12RB1, ISG15, IFNGR1, IFNGR2, STAT1, and IRF8) and two X-linked mutations (in IKBKG and CYBB), mostly presenting in childhood, have been reported to confer susceptibility to disseminated non-tuberculous mycobacterial infection. GATA2 defi ciency and antiinterferon γ autoantibodies also give rise to disseminated infection, typically in late childhood or adulthood. Furthermore, isolated pulmonary non-tuberculous mycobacterial infection has been increasing in prevalence in people without recognised immune dysfunction. In this Review, we discuss how to detect and diff erentiate host susceptibility factors underlying localised and systemic non-tuberculous mycobacterial infections.

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“…Production of IFN-γ by activated T and natural killer cells is under the control of IL-12 and IL-23, which are secreted by activated macrophages. Mutations of IL-12 p40, IL-12 receptor β-1 subunit, IFN-γ receptor 1, IFN-γ receptor 2 and of the signaling molecule STAT1 have been shown to cause genetically determined susceptibility to mycobacterial disease in humans, in which dissemination to lungs is common and often fatal [103, 104]. …”

Section: Lung Disease In Other Immunodeficienciesmentioning

confidence: 99%

Genetic Causes of Bronchiectasis: Primary Immune Deficiencies and the Lung

Notarangelo

Plebani²,

Mazzolari³

et al. 2007

Respiration

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Primary immune deficiencies (PID) comprise a heterogeneous group of genetically determined disorders that affect development and/or function of innate or adaptive immunity. Consequently, patients with PID suffer from recurrent and/or severe infections that frequently involve the lung. While the nature of the immune defect often dictates the type of pathogens that may cause lung infection, there is substantial overlap of radiological findings, so that appropriate laboratory tests are mandatory to define the nature of the immune defect and to prompt appropriate treatment. At the same time, the recent identification of a large number of PID-causing genes now allows early, even presymptomatic diagnosis, thus representing an essential tool for prevention of lung damage. This review article describes the most common forms of PID, their cellular and molecular bases, and the associated lung abnormalities, and reports on available treatment.

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Disseminated <i>Mycobacterium avium</i> Infection in a 20-Year-Old Female with Partial Recessive IFNγR1 Deficiency

Cited by 46 publications

References 31 publications

Adjuvant modulation of the cytokine balance in Mycobacterium tuberculosis subunit vaccines; immunity, pathology and protection

Adjuvant modulation of the cytokine balance in Mycobacterium tuberculosis subunit vaccines; immunity, pathology and protection

Host susceptibility to non-tuberculous mycobacterial infections

Genetic Causes of Bronchiectasis: Primary Immune Deficiencies and the Lung

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