Enhanced Phagocytic Activity of HIV-Specific Antibodies Correlates with Natural Production of Immunoglobulins with Skewed Affinity for FcγR2a and FcγR2b

Ackerman, Margaret E.; Dugast, Anne‐Sophie; McAndrew, Elizabeth; Tsoukas, Stephen; Licht, Anna; Irvine, Darrell J.; Alter, Galit

doi:10.1128/jvi.03403-12

Cited by 86 publications

(100 citation statements)

References 59 publications

(69 reference statements)

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“…Since then, patient studies support the notion that IgG glycosylation directly impacts function. For autoimmunity, terminal galactosylation (27) and terminal sialylation (2-4, 6) are now established factors in immune modulation, whereas fucosylation has been shown to correlate with antibody-dependent cell-mediated viral inhibition (ADCVI) activity in the context of HIV infection (28,29) as well as antibody-dependent cellular cytotoxicity (ADCC) in vitro (30). For ADCC, structural rearrangements associated with the presence of fucose within the Fc domain appear to account for the functional shift (31), but it remains unclear how fucosylation translates into differential ADCVI activity.…”

Section: Discussionmentioning

confidence: 99%

B-cell–independent sialylation of IgG

Jones

Oswald

Joshi

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

117

107

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IgG carrying terminal α2,6-linked sialic acids added to conserved N-glycans within the Fc domain by the sialyltransferase ST6Gal1 accounts for the anti-inflammatory effects of large-dose i.v. Ig (IVIg) in autoimmunity. Here, B-cell-specific ablation of ST6Gal1 in mice revealed that IgG sialylation can occur in the extracellular environment of the bloodstream independently of the B-cell secretory pathway. We also discovered that secreted ST6Gal1 is produced by cells lining central veins in the liver and that IgG sialylation is powered by serum-localized nucleotide sugar donor CMP-sialic acid that is at least partially derived from degranulating platelets. Thus, antibody-secreting cells do not exclusively control the sialylationdependent anti-inflammatory function of IgG. Rather, IgG sialylation can be regulated by the liver and platelets through the corresponding release of enzyme and sugar donor into the cardiovascular circulation.W hile en route to the plasma membrane as integral membrane proteins or for secretion, glycoproteins exiting the endoplasmic reticulum traverse the cis-, medial-, and trans-Golgi apparatus where the associated N-linked glycans are remodeled into their final form. This classically defined secretory pathway dictates that the glycoform of all glycoproteins produced by a cell is largely determined by the cohort of enzymes within the Golgi and the metabolic circumstances of that specific cell.Protein glycosylation is known to play fundamental roles in all aspects of biology, but has recently gained significant attention in immunology. When administered at high doses, i.v. Ig (IVIg) is an effective anti-inflammatory treatment for autoimmune patients (1). In 2006, it was discovered that the ∼10% of IgG molecules that carry α2,6-linked sialic acids upon the conserved biantennary N-glycans within the Fc domain provided the potent IVIg anti-inflammatory activity in autoimmune disease (2). Indeed, enrichment for the sialylated IgG (sIgG) fraction from IVIg pools increased the efficacy of treatment in mouse models of arthritis 100-fold in an IL-4-dependent fashion through receptors such as CD209 (DC-SIGN) (3, 4). Moreover, it was reported that sialylation of IgG also impacts antibody affinity maturation, although the mechanism underlying this phenomenon remains to be fully elucidated (5). These data indicate that sialylation serves as the mechanism underlying pleotropic IgG function (3,4,6).Epidemiologic analyses published since the reports cited above are consistent with this model. For example, female rheumatoid arthritis patients often go into remission during pregnancy and then relapse following childbirth. Analysis of sIgG levels before, during, and after pregnancy showed that the level of sIgG increases rapidly during pregnancy-induced remission, whereas during periods of exacerbated disease, sIgG is essentially undetectable (7,8). To date, it is unclear whether IgG sialylation patterns precede or result from the inflammatory state, and essentially nothing is known about the regulatory mecha...

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Section: Discussionmentioning

confidence: 99%

B-cell–independent sialylation of IgG

Jones

Oswald

Joshi

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

117

107

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“…Analysis of the rare HIV-1 infected subjects who naturally completely control viral replication (termed "elite controllers") also illustrate the integral role that ADCC and ADCP play in natural immunity. The trend observed in several studies of natural infection was for higher levels of ADCC antibodies and a response skewed to IgG3/1 subclasses in HIV-1 controllers compared to an IgG4/2 subclass skewing in viremic individuals [18,61,71,72]. ADCC-antibodies are produced more rapidly following infection than neutralizing antibodies, which typically take months or years to develop [46,49].…”

Section: In Vivo Studies Iii: Natural Infectionmentioning

confidence: 98%

“…Forthal et al (2001) found plasma from acutely infected patients and normal NK effector cells were able to inhibit viral replication, suggesting a role for antibody and NK cells in early control of infection [68]. The assay can use NK cells or monocytes for killing of infected targets [18]. Other formats measured Fc-dependent direct inhibition of replication in primary macrophages [20].…”

Section: Cell Based Functional Assays For Fcr Activating Antibodiesmentioning

confidence: 99%

“…The normal ligands for cellular FcγR interactions are complexes of IgG and increased complex size increases the avidity of interaction and binding activity [165]. Therefore more functional antigenspecific assays measure binding of complexes to immobilised recombinant soluble receptors [18,166]. For example, recombinant soluble FcγR ectodomains with c-terminal hexahistidine tags have been immobilised on plates via antihexahistidine mAb [166] or nickel [18] to produce an array of receptors for binding IgG ligands.…”

Section: Fcγr Binding Assaysmentioning

confidence: 99%

“…Importantly, there is evidence that each activating FcγR can contribute to some protective effects of anti-HIV antibodies (e.g. [18][19][20][21][22][23]). Aggregation of cellular Fc receptors [24], or possibly their reorganisation in the membrane [25] leads to the activation of src family and syk kinases which initiate a cell activation cascade and, depending on the innate cell type, stimulate effector functions such as ADCC and ADCP [1][2][3]26].…”

Section: Introductionmentioning

confidence: 99%

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Antibody functional assays as measures of Fc receptor-mediated immunity to HIV - new technologies and their impact on the HIV vaccine field.

Wines¹,

Billings²,

Mcleand³

et al. 2017

CHR

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Background:There is now intense interest in the role of HIV-specific antibodies and the engagement of FcγR functions in the control and prevention of HIV infection. The analyses of the RV144 vaccine trial, natural progression cohorts, and macaque models all point to a role for Fc-dependent effector functions, such as cytotoxicity (ADCC) or phagocytosis (ADCP), in the control of HIV. However, reliable assays that can be reproducibly used across different laboratories to measure Fcdependent functions, such as antibody dependent cellular cytotoxicity (ADCC) are limited. Method: This brief review highlights the importance of Fc properties for immunity to HIV, particularly via FcγR diversity and function. We discuss assays used to study FcR mediated functions of HIV-specific Ab, including our recently developed novel cell-free ELISA using homo-dimeric FcγR ectodomains to detect functionally relevant viral antigen-specific antibodies. Results: The binding of these dimeric FcγR ectodomains, to closely spaced pairs of IgG Fc, mimics the engagement and cross-linking of Fc receptors by IgG opsonized virions or infected cells as the essential prerequisite to the induction of Ab-dependent effector functions. The dimeric FcγR ELISA reliably correlates with ADCC in patient responses to influenza. The assay is amenable to high throughput and could be standardized across laboratories. Conclusion: We propose the assay has broader implications for the evaluation of the quality of antibody responses in viral infections and for the rapid evaluation of responses in vaccine development campaigns for HIV and other viral infections.

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A Dual‐domain Engineered Antibody for Efficient HBV Suppression and Immune Responses Restoration

Jiang,

Chen,

et al. 2024

Advanced Science

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Chronic hepatitis B (CHB) remains a major public health concern because of the inefficiency of currently approved therapies in clearing the hepatitis B surface antigen (HBsAg). Antibody‐based regimens have demonstrated potency regarding virus neutralization and HBsAg clearance. However, high dosages or frequent dosing are required for virologic control. In this study, a dual‐domain‐engineered anti‐hepatitis B virus (HBV) therapeutic antibody 73‐DY is developed that exhibits significantly improved efficacy regarding both serum and intrahepatic viral clearance. In HBV‐tolerant mice, administration of a single dose of 73‐DY at 2 mg kg−1 is sufficient to reduce serum HBsAg by over 3 log10 IU mL−1 and suppress HBsAg to < 100 IU mL−1 for two weeks, demonstrating a dose‐lowering advantage of at least tenfold. Furthermore, 10 mg kg−1 of 73‐DY sustainably suppressed serum viral levels to undetectable levels for ≈ 2 weeks. Molecular analyses indicate that the improved efficacy exhibited by 73‐DY is attributable to the synergy between fragment antigen binding (Fab) and fragment crystallizable (Fc) engineering, which conferred sustained viral suppression and robust viral eradication, respectively. Long‐term immunotherapy with reverse chimeric 73‐DY facilitated the restoration of anti‐HBV immune responses. This study provides a foundation for the development of next‐generation antibody‐based CHB therapies.

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Enhanced Phagocytic Activity of HIV-Specific Antibodies Correlates with Natural Production of Immunoglobulins with Skewed Affinity for FcγR2a and FcγR2b

Cited by 86 publications

References 59 publications

B-cell–independent sialylation of IgG

B-cell–independent sialylation of IgG

Antibody functional assays as measures of Fc receptor-mediated immunity to HIV - new technologies and their impact on the HIV vaccine field.

A Dual‐domain Engineered Antibody for Efficient HBV Suppression and Immune Responses Restoration

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