Antibody Formation Initiated in Vitro

Fishman, Marvin A.; Adler, Frank L.

doi:10.1084/jem.117.4.595

Cited by 309 publications

(41 citation statements)

References 11 publications

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“…Glasgow [10] presented the results that antiserum-treated cells had only a low capacity of IF production and neutralized [2,5] and that macrophages have a specific receptor for this antibody [12]. Mitsuhashi et al [16] have discussed that the macrophages have three functions in defense mechanism; the first function is phagocytosis, the second being production of transfer agent which transfers immunogenic information to immunocompetent cells [9,13], and the third is for the production of cellular antibody [14]. The mechanism of enhancement of IF production in macrophages will be also analyzed from the point of view of cytophilic antibody and cellular antibody.…”

Section: Discussionmentioning

confidence: 99%

Relationship between Immunity and Interferon Production in Macrophages

Azuma

Yamada

Nishioka

1970

Japanese Journal of Microbiology

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The effect of antiserum on the interferon (IF) production in macrophages by Newcastle disease virus (NDV) has been studied. Completely neutralized NDV lost its IF-inducing ability, but under-neutralized NDV revealed an enhanced IFinducing capability. This enhancement of IF production by unneutralized NDV was also observed in antiserum-treated cells. Enhancement phenomena appeared to be based on immunological specificity. Under-neutralized NDV was also adsorbed more rapidly and at a higher rate to normal cells than unneutralized NDV. Unneutralized NDV also adsorbed more efficiently to antiserum-treated cells and to cells derived from immunized mice than to normal cells. The significance of these phenomena is discussed in relation to the induction mechanism of IF in macrophages.

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Section: Discussionmentioning

confidence: 99%

Relationship between Immunity and Interferon Production in Macrophages

Azuma

Yamada

Nishioka

1970

Japanese Journal of Microbiology

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“…The size may affect the period within the body during which an antigen may retain its configuration and may also affect the rate at which it is phagocytized. Whether such phagocytosis is itself an active step in the initiation of the immune response (37,38) it simply serves to reduce the ambient antigen concentration in the immediate surroundings of antibody-forming cells must remain open. Promoting capacity of cells does not solely depend on size of the antigen: the promoting capacity of red blood corpuscles and nucleated cells shows considerable differences.…”

Section: Discussionmentioning

confidence: 99%

Cells as Antigen Carriers and as Immunoglobulin Producers

Chou

Dubiski

Cinader

1967

The Journal of Experimental Medicine

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Tolerance induction and antibody formation appear to be alternative consequences of exposure to antigen. The decision between the alternatives depends, on the one hand, on the dose (1, 2), structure (3), and molecular weight (4, 5) of the antigen and, on the other, on the age, species, and immunological status of the recipient. While some of the factors which cause tolerance in adult animals have been explored in detail, little is known about the conditions which promote antibody formation after neonatal exposure to an antigen. To explore this further, we have injected newborn rabbits with small quantities of human albumin (HA) either in soluble form or in association with rabbit cells. The protein was either linked to rabbit erythrocytes by covalent bonds or taken up by nucleated ceils from the thymus, the lymph nodes, the peritoneal cavity, or the lungs. The cellular origin of antibody was determined by allotypic markers on the antibody molecules. The fate of the transferred cells in the recipient animal was followed by monitoring the ailotypic markers of the circulating immunoglobulin molecules. Materials and MethodsGlycogen.--Glycogen of cp grade was obtained from Pfanstlehl Chemical Co., Waukegan, Ill., and Fish Reagent Chemical Glycogen was obtained from Fish Scientific Co., New York. A 1% (w/v) stock solution of glycogen in glass-distilled water was prepared and was sterilized by steaming at 100°C for 30 rain daily for 3 consecutive days. Immediately before use a 0.1% solution was prepared from this sterile stock solution by adding 100 ml of the 1% solution to 900 ml of Baxter sterile nonpyrogenic normal saline (Baxter

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“…The observations with the polylysine hapten conjugates and the copolymers of GA and GL strongly suggest that besides the recognition of the antigenic determinant capable of inducing specific antibody synthesis, an earlier step of metabolism of the antigen molecule must take place, presumably at the level of the macrophages, for the inducer to be made (9,10). Recent observations of Maurer (11) and Gill et o2.…”

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confidence: 93%

Studies on Artificial Antigens

Benacerraf

Ojeda

Maurer

1963

The Journal of Experimental Medicine

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An effort was made to immunize guinea pigs with arsanilic acid conjugates of copolymers of D- and L-α-amino acids; ASD-GAT and ASL-GAT. An immune response was observed only in the case of ASL-GAT. Antibodies specific for the arsanilic acid hapten were produced which could also react with ASD-GAT or ASGPA. These findings indicate that the proper metabolism of the antigen may be essential to the induction of the immune response.

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Antibody Formation Initiated in Vitro

Cited by 309 publications

References 11 publications

Relationship between Immunity and Interferon Production in Macrophages

Relationship between Immunity and Interferon Production in Macrophages

Cells as Antigen Carriers and as Immunoglobulin Producers

Studies on Artificial Antigens

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