Affinity Tag Coating Enables Reliable Detection of Antigen-Specific B Cells in Immunospot Assays

Köppert, Sebastian; Wolf, Carla; Becza, Noémi; Franke, Fridolin; Küerten, Stefanie; Ross, Ted M.; Lehmann, Paul; Kirchenbaum, Greg A.

doi:10.3390/cells10081843

Cited by 13 publications

(16 citation statements)

References 101 publications

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“…While the methodology for the quantification of antigen-reactive antibodies in plasma by ELISA is well-established, we first needed to develop such for the objective and accurate counting of antigen-reactive B mem cells in the blood. Empirically, antigen-reactive B cell ImmunoSpot ® assays result in diverse spot morphologies [ 47 ] (see also Figure 1 B,C). This outcome is expected as the secretory footprints of individual ASCs are defined by a multitude of parameters [ 61 ] including (a) the net amount of antibodies produced by the individual B cells during the assay’s duration, (b) the kinetics of antibody production by the ASCs, and (c) the functional affinity of each ASC’s antibody for the antigen (that can encompass a broad spectrum among an antigen-reactive B cell repertoire, defining the capture and dissociation rates of antibodies binding to antigens).…”

Section: Resultsmentioning

confidence: 99%

“…For the enumeration of antigen-reactive IgG + ASCs, ImmunoSpot ® assays were performed with ACC as previously described [ 47 ] and illustrated by Figure S1 . Briefly, assay plates were first preconditioned with 70% ( v / v ) EtOH followed by two washing steps with PBS.…”

Section: Methodsmentioning

confidence: 99%

“…Successful coating therefore depends on the physical properties of the membrane chosen versus the corresponding properties of the antigen itself. To overcome this limitation in the development of B cell ImmunoSpot ® assays for “any antigen of interest”, we recently introduced an approach termed “affinity capture coating” (ACC) in which improved antigen absorption to the membrane is achieved through preconditioning the assay membrane with an antibody specific for the genetically encoded hexahistidine (6XHis) affinity tag of the recombinant proteins [ 47 ], enabling the subsequent high-affinity capture of any 6XHis-tagged protein. Using this universal ACC approach, we developed ImmunoSpot ® assays that enable the detection of memory B cells reactive with antigens representing SARS-CoV-2, seasonal influenza, and Epstein–Barr virus (EBV) [ 47 ].…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Antibody Levels Poorly Reflect on the Frequency of Memory B Cells Generated following SARS-CoV-2, Seasonal Influenza, or EBV Infection

Wolf

Köppert

Becza³

et al. 2022

Cells

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The scope of immune monitoring is to define the existence, magnitude, and quality of immune mechanisms operational in a host. In clinical trials and praxis, the assessment of humoral immunity is commonly confined to measurements of serum antibody reactivity without accounting for the memory B cell potential. Relying on fundamentally different mechanisms, however, passive immunity conveyed by pre-existing antibodies needs to be distinguished from active B cell memory. Here, we tested whether, in healthy human individuals, the antibody titers to SARS-CoV-2, seasonal influenza, or Epstein–Barr virus antigens correlated with the frequency of recirculating memory B cells reactive with the respective antigens. Weak correlations were found. The data suggest that the assessment of humoral immunity by measurement of antibody levels does not reflect on memory B cell frequencies and thus an individual’s potential to engage in an anamnestic antibody response against the same or an antigenically related virus. Direct monitoring of the antigen-reactive memory B cell compartment is both required and feasible towards that goal.

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Antibody Levels Poorly Reflect on the Frequency of Memory B Cells Generated following SARS-CoV-2, Seasonal Influenza, or EBV Infection

Wolf

Köppert

Becza³

et al. 2022

Cells

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“…Recently, we concluded a systematic study (to the best of our knowledge the rst on this subject) in which we measured circulating antibody levels to SARS-CoV-2, EBV, and different seasonal in uenza virus strains and compared them with the frequencies of B mem reactive with the same antigens [6]. These ImmunoSpot®-based B mem detections were enabled by our newly-acquired ability to achieve high density antigen coating, thus reliable detection of B mem speci c for essentially any antigen ( [11] and Note 8).…”

Section: Emerging Evidence For Serum Antibody Levels and Memory Cell ...mentioning

confidence: 99%

“…Consequently, many investigators likely gave up on this assay after not being successful in their initial attempts to establish such assays for the antigen(s) of interest. Our recent introduction of a nity capture coating [11] represents a breakthrough to this end, as it provides a universal strategy for successful assay development for essentially any antigen: the membrane is rst coated with an anti-(His-or other) a nity tag-speci c antibody followed by the addition of recombinant (His-or other) a nity-tagged recombinant antigen. In this way, low-a nity absorption of the antigen to the membrane via weak, non-speci c binding forces (primarily hydrophobicity) is replaced by speci c, high-a nity binding.…”

Section: Emerging Evidence For Serum Antibody Levels and Memory Cell ...mentioning

confidence: 99%

Monitoring memory B cells by next generation ImmunoSpot® provides insights into humoral immunity that measurements of circulating antibodies do not reveal

Lehmann,

Liu,

Becza

et al. 2023

Preprint

Self Cite

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Memory B cells (Bmem) provide the second wall of adaptive humoral host defense upon specific antigen rechallenge when the first wall, consisting of pre-formed antibodies originating from a preceding antibody response, fails. This is the case, as recently experienced with SARS-CoV-2 infections and previously with seasonal influenza, when levels of neutralizing antibodies decline or when variant viruses arise that evade such. While in these instances reinfection can occur, in both scenarios, the rapid engagement of preexisting Bmem into the recall response can still confer immune protection. Bmem are known to play a critical role in host defense, yet their assessment has not become part of the standard immune monitoring repertoire. Here we describe a new generation of B cell ELISPOT/FluoroSpot (collectively ImmunoSpot®) approaches suited to dissect, at single-cell resolution, the Bmem repertoire ex vivo, revealing its immunoglobulin class/subclass utilization, and its affinity distribution for the original, and for variant viruses/antigens. Because such comprehensive B cell ImmunoSpot® tests can be performed with minimal cell material, are scalable, and robust, they promise to be well-suited for routine immune monitoring.

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Monitoring Memory B Cells by Next-Generation ImmunoSpot® Provides Insights into Humoral Immunity that Measurements of Circulating Antibodies Do Not Reveal

Lehmann,

Liu,

Becza

et al. 2024

Methods in Molecular Biology

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Memory B cells (Bmem) provide the second wall of adaptive humoral host defense upon specific antigen rechallenge when the first wall, consisting of preformed antibodies originating from a preceding antibody response, fails. This is the case, as recently experienced with SARS-CoV-2 infections and previously with seasonal influenza, when levels of neutralizing antibodies decline or when variant viruses arise that evade such. While in these instances, reinfection can occur, in both scenarios, the rapid engagement of preexisting Bmem into the recall response can still confer immune protection. Bmem are known to play a critical role in host defense, yet their assessment has not become part of the standard immune monitoring repertoire. Here we describe a new generation of B cell ELISPOT/FluoroSpot (collectively ImmunoSpot®) approaches suited to dissect, at single-cell resolution, the Bmem repertoire ex vivo, revealing its immunoglobulin class/subclass utilization, and its affinity distribution for the original, and for variant viruses/antigens. Because such comprehensive B cell ImmunoSpot® tests can be performed with minimal cell material, are scalable, and robust, they promise to be well-suited for routine immune monitoring.

show abstract

Affinity Tag Coating Enables Reliable Detection of Antigen-Specific B Cells in Immunospot Assays

Cited by 13 publications

References 101 publications

Antibody Levels Poorly Reflect on the Frequency of Memory B Cells Generated following SARS-CoV-2, Seasonal Influenza, or EBV Infection

Antibody Levels Poorly Reflect on the Frequency of Memory B Cells Generated following SARS-CoV-2, Seasonal Influenza, or EBV Infection

Monitoring memory B cells by next generation ImmunoSpot® provides insights into humoral immunity that measurements of circulating antibodies do not reveal

Monitoring Memory B Cells by Next-Generation ImmunoSpot® Provides Insights into Humoral Immunity that Measurements of Circulating Antibodies Do Not Reveal

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