Circulating Antibody Response Research Articles

Nasal and circulating antibody responses to influenza vaccination and their importance in resistance to infection.

Summary Small groups of volunteers were inoculated intranasally with live-attenuated, and parenterally with detergent-split-saline or with whole-virus-oil-adjuvant influenza A2/HK (H3N2) vaccines after the prevalence of Hong Kong strains. Antibody titres in nasal secretions and serum were measured by HI, antineuraminidase and neutralization tests. The oil adjuvant vaccine produced large rises in antibodies and the other two vaccines produced small rises. The volunteers given oil adjuvant and live vaccine were both well protected against challenge with a partly attenuated strain. Statistical analysis showed that resistance to infection was predicted best by high titres of antibody in the serum, but the presence of antibody did not seem to explain completely resistance to infection.

A small-scale feeding trial of an attenuated type 3 poliovirus USOL-D bac vaccine (author's transl)

A small-scale trial of an attenuated type 3 poliovirus vaccine prepared with the USOL-D bac strain was carried out as a part of the collaborative study under the WHO's auspices.In two closed institutions 26 children 5 to 13 months of age who had no history of anti-polio vaccination were administered with the vaccine, and 10 children of similar ages were left unvaccinated as room contacts. Of all the children, 21 vaccinees and 5 contacts had no circulating antibody against polioviruses. Most of the children in one institution (Infant Home H) excreted type 2 adenovirus in stools before or during the trial. No viral agent was isolated from pre-trial stools collected in the other institution (Infant Home B).Inoculated with a single dose of the vaccine containing105.8 TCD50 of the virus, the vaccinees in both institutions excreted considerably large amounts of type 3 poliovirus for long periods. One child in Infant Home B showed only transient excrection of the minimal detectable amount of virus on day 8. In Infant Home H the longest duration of virus excretion was 41 days with an average excretion period of 33.6 days, while in Infant Home B the longest duration of excretion was not less than 85 days with an average of 61.4 days. There was, however, no such great difference in the average of the maximal virus content per gram of stool of individual children between the two infant homes. This average was 107.4 TCD50 in the H institution and 107.1 TCD50 in the B. Stools of the contact children were examined only in Infant Homes H, where only one contact child excreted a small amount of virus on day 6.Circulating antibody response was good in all the vaccinees, except the one mentioned above in Infant Home B. This child and three contacts of Infant Home H, including the one mentioned above, showed no rise of circulating antibody. The contacts of Infant Home B were fed Sabin types 1 and 2 divalent vaccine one week after the commencement of the trial, but they showed only type 3 antibody response. This may indicate that efficient contact infection with the vaccine virus took place during the first week of the trial.Reversion of rct/40 character of virus progeny was observed rather early, and 45per cent of the isolates investigated was positive for rct/40 character, while only 14per cent was negative. The incidence of reversion appeared irregularly in individual children. Some children excreted rct/40± of ract/40+ virus early and again excreated rct/40- virus later.The results obtained indicated that the USOL-D bac virus multiplied well in the gut of children, who showed a good antibody response, although it was genetically unstable. Efficient contact infection was observed in one institution where children were in close contact with one another in a play-room. Contact infection was almost completely prevented in the other institution where children were kept in bed.The USOL-D bac virus was discussed for suitability as a candidate for a more acceptable type 3 poliovirus vaccine strain, in comparison with the Sabin type 3 Leon 12a1b virus.

An experimental epidemiological study of Talfan virus infection in pigs

Talfan virus was introduced experimentally into a small herd of MD pigs by the oral dosing of one litter of piglets with virus cultivated in PK cells. Serum samples from all pigs in the herd were examined for Talfan neutralizing antibodies at monthly intervals for 8 months, and virus isolation from rectal swabs was attempted at weekly or monthly intervals for the same period. Samples from the colon were collected for virus isolation from pigs at slaughter. The infection produced diarrhoea in suckling piglets and in one gilt, and nervous signs in suckling piglets, one gilt and one boar during the first 5 weeks of the experiment. Thereafter, clinical disease attributed to Talfan virus was not apparent. In the early (epidemic) phase of the infection, pigs of all ages excreted virus for a period up to 8 weeks and developed circulating antibodies which persisted at fairly high levels throughout the experiment. Piglets born one month or more after the introduction of Talfan virus excreted virus only after weaning and developed a circulating antibody response to Talfan in the post-weaning period.

Immunosuppression by procarbazine: I. Sites of action of the drug and effect on adjuvant arthritis and circulating antibody responses

The effect of procarbazine hydrochloride on adjuvant arthritis and on circulating antibody responses in the rat was studied. Procarbazine had a profoundly depressing effect on both adjuvant arthritis and the circulating antibody response to ovalbumin (OA). In contrast, it had no effect on the immune response to sheep erythrocytes (SRBC) alone; the presence of adjuvant, however, enhanced the response to SRBC, and this enhancement was suppressed by procarbazine. Preinjection with adjuvant enhanced the response to OA given at a different site: procarbazine treatment at the time of adjuvant injection suppressed this enhancement. These results taken in conjunction with histological observations, reinforce the idea that the initial effect of the drug is predominantly on the thymus and thymus-dependent cell populations, though prolonged treatment may also affect the bone marrow. They also give a clue to the mode of action of adjuvant in enhancing immune responsiveness. It is suggested that judicious use of procarbazine may assist fine dissection of various components of the immune response.

Comparison of antibody responses in normal and alloxan diabetic mice.

The reason for the increased incidence and severity of infections in diabetic patients has never been satisfactorily explained. This investigation was designed to study the circulating antibody response in alloxan diabetic, insulin treated diabetic and normal CF-1 mice injected with bovine serum albumin. Only those animals treated with alloxan who had elevated serum glucose levels (250 mg./100 ml. or higher) were included in the study, together with a group of normal animals. Animals were bled from the orbital sinus and the serum analyzed for antigen binding capacity of BSA, glucose concentration and serum proteins. BSA was iodinated with I-131 and the antigen binding capacity of each serum sample was determined as micrograms of BSA nitrogen bound by 1 ml. of undiluted serum. Our studies demonstrate that there is no significant difference in antibody response of alloxan treated mice, alloxan treated mice given insulin and normal mice when immunized with BSA under the conditions of the experiments. If the alloxan treated mouse may be considered a laboratory model of diabetes mellitus in man, the results described herein would be consistent with those studies of diabetics which have shown no primary defect in their immune systems.

Agar-Gel Precipitating Antibody in Pseudomonas aeruginosa Infections

The human immune response to Pseudomonas aeruginosa infection was studied by using the double diffusion in agar-gel technique. Antigens from Fisher-Devlin-Gnabasik immunotypes were prepared by both trichloroacetic acid extraction and ultrasonic disruption. Serum from 72 of 168 patients (43%) from whom P. aeruginosa was isolated formed from one to eight precipitin bands. Precipitins were demonstrated in the sera of 60 of 66 (91%) patients recovering from bacteremia and deep infections; however, they were usually absent when Pseudomonas infection was fatal or when there was no clinical evidence of significant infection. Precipitating antibody was detectable at serum dilutions as high as 1:32, and appearance of single bands correlated with hemagglutinating antibody titers of >/=1:128. Antigen from sonically disrupted organisms usually resulted in stronger precipitin bands than trichloroacetic acid extracts, and antigen from the homologous infecting strain occasionally increased test sensitivity. None of 50 normal controls had Pseudomonas precipitins as was the case in patients convalescing from Escherichia coli (15 patients), Klebsiella-Enterobacter-Serratia (18), and Proteus (14) bacteremias. Measurement of agar-gel precipitins was useful and specific in evaluating the circulating antibody response to P. aeruginosa infections.

The Effect of X-Irradiation on Delayed Hypersensitivity and Circulating Antibody in the Rat

Abstract Rats exposed to x-radiation 24 hr before antigen administration exhibited detectable skin reactions to tuberculin 2 days later than nonirradiated sensitized controls. Reaction sizes illustrate that the irradiated rat experienced a decreased sensitivity to tuberculin which persisted through day 14. The radiation dose (475 rads) responsible for the observed depression of the delayed skin reactions produced a greater depression of the circulating antibody response. The results obtained suggest that the cellular and humoral immune responses in the rat are radiosensitive.

The effect of tumour growth on immune competence. A study of DMBA mammary carcinogenesis in the rat.

Circulating antibody response to flagella antigen has been measured in three groups of Sprague-Dawley rats after feeding with 7.12.DMBA in an attempt to differentiate carcinogen and tumour growth as causative agents in the depression of immune response seen in these animals. DMBA fed female rats developing tumours had progressive depression of both primary and secondary response as compared to control animals, and 7S and 19S antibody fractions were equally affected. Removal of tumours did not result in recovery of response. Attempts to prevent tumour development by mammectomy after DMBA feeding were unsuccessful, but the similar number of tumours found in this group was associated with an equal degree of antibody depression to that seen in the first experiment. Male animals fed DMBA did not develop malignant tumours, and showed no depression of immune response. Results suggest that tumour development plays a part in the depression of circulating antibody response seen in these animals, but that it is not directly related to the number of tumours, and is not reversible by tumour excision.

Isologous and Homologous Lymphoid Transplants

Summary Stimulation of guinea pigs with protein antigen incorporated in complete Freund's adjuvant results in sequential production of three types of immunoglobulins. The initial response of rapidly sedimenting or macroglobulin antibody is superseded by a γ1 (PCA) 7 S antibody response. Subsequently the γ2 (cytotoxic) 7 S antibody appears in significant amounts. This last stage signals full maturation of the circulating antibody response so far as it can be measured by current techniques. By extirpation of the stimulated regional lymph nodes at discrete intervals during the differentiation process and injection of the dispersed cells into isologous normal recipients, the various stages of the primary immune response can be isolated and studied. In the absence of additional antigen, the types of antibody detectable in the donor at the time of transfer are the only kinds produced in the recipient. The possible mechanism of this arrest of maturation and the application of this model system are discussed.

Induction of Tuberculin Hypersensitivity and Serologic Unresponsiveness to Tubercle Bacilli in Newborn and Young Cuinea Pigs

Summary The age at sensitization with tubercle bacilli was shown to have a marked influence on the expression of tuberculin skin reactivity in young guinea pigs. Animals varying in age from 0 to 4 weeks old were injected with 5 mg (dry weight) of heat-killed M. tuberculosis (H37Rv strain) and skin tested 2 weeks later with 5 µg of PPD. Only the 4-week-old animals exhibited tuberculin hypersensitivity to the same degree as similarly-sensitized adult animals. Evidence was provided to indicate that the failure of the younger animals to exhibit skin reactivity may reflect a nonspecific deficiency of the skin rather than a fault in functional immune capacity. The effect of varying the size of the sensitizing dose on tuberculin skin reactivity was not as striking as varying the age at sensitization. Positive skin reactions were noted following the use of sensitizing doses ranging from 0.125 mg to 5.0 mg when the animals were skin tested 2 weeks after injection. In contrast, the serologic reactivity of the sensitized young animals decreased as the sensitizing dose was increased above 0.5 mg. The 5-mg dose was found to induce serologic unresponsiveness quite effectively in newborn animals. Serologic unresponsiveness represented at least a 100-fold decrease in the circulating antibody response. It was suggested that serologic unresponsiveness may reflect a form of specific immune suppression. The implications of these findings to the use of acquired immunologic tolerance in guinea pigs as a model for study of the mechanisms of immunity in tuberculosis are discussed.

Passive hemolytic antibody response of primed, partially resistant mice to heat-killed Salmonella typhimurium vaccine.

SummaryMean effective doses (50% protection) of S. typhimurium heat-killed, alcohol-treated bacterial vaccine depended upon the interval before challenge at which the single dose was given. Circulating antibody response against the lipopolysaccharide component of the organism appeared to be related to the magnitude of the mean effective dose, but not to the partial immunity developed. Killed vaccine was an effective immunizing agent if given at an optimal time interval before challenge.

Intestinal lymphangiectasia

Intestinal lymphangiectasia is a disease characterized by dilated intestinal lymphatics, protein-losing enteropathy, hypoalbuminemia, and edema. The immunologic status of 18 patients with intestinal lymphangiectasia was studied. Concentrations of IgG, IgA, and IgM were measured by immune precipitation and metabolism of these three immunoglobulins was studied using purified radioiodinated proteins. The serum concentration and total body pool of each immunoglobin were greatly reduced. The fraction of the intravascular protein pool catabolized per day was increased to 34% for IgG, 59% for IgA, and 66% for IgM; these are in contrast with control values of 7%, 28%, and 17%, respectively. Synthetic rates of the immunoglobulins were normal or slightly increased. Primary circulating antibody response was tested in five patients with Vi and tularemia antigens. Titers elicited in patients with the Vi antigen were significantly lower than those seen in a control group, whereas no difference was seen between patient and control responses to the tularemia antigen. Lymphocytopenia was noted in patients with intestinal lymphangiectasia. The mean circulating lymphocyte count was 710 +/- 340/mm(3) in contrast to 2500 +/- 600/mm(3) in controls. Cellular hypersensitivity was studied with skin tests and skin grafts. 91% of normal individuals reacted to at least one of the four skin test antigens: purified protein derivative, mumps, Trichophyton, and Candida albicans; in contrast, only 17% of patients with intestinal lymphangiectasia had a positive reaction. Each of three patients tested with dinitrochlorobenzene had a negative reaction. Finally, all four patients who received skin homografts have retained these grafts for at least 12 months. The immunological disorders in patients with intestinal lymphangiectasia appear to result from loss of immunoglobulins and lymphocytes into the gastrointestinal tract secondary to disorders of lymphatic channels. Lymphocyte depletion then leads to skin anergy and impaired homograft rejection.

Hereditary alterations in the immune response: coexistence of "agammaglobulinemia", acquired hypogammaglobulinemia and selective immunoglobulin deficiency in a sibship.

Extract: A longitudinal immunologic study was conducted in a family in which an entire sibship of three males was unduly susceptible to infection. The oldest boy's history of repeated severe infections beginning in infancy and his marked deficiencies of all three major immunoglobulins were compatible with a clinical diagnosis of congenital ‘agammaglobulinemia' (table I, fig. 1). Recurrent severe infections in the second boy did not begin until late childhood, and his serum abnormality involved deficiencies of only two of the major immunoglobulin fractions, IgG and IgM (table I, fig. 1). This phenotype of selective immunoglobulin deficiency is previously unreported. Serum concentrations of the three immunoglobulins in the youngest boy (who also had a late onset of repeated infection) were normal or elevated when he was first studied, but a marked decline in levels of each of these fractions was observed over a four-year period (table I, fig. 1). We could find no previous reports describing apparent congenital and acquired immunologic deficiencies in a sibship. Repeated infections and demonstrated specific immunologic unresponsiveness preceded gross abnormalities in the total and fractional gamma globulin levels in both of the younger boys (tables II–IV). When the total immunoglobulin level in the second boy was 735 mg/100 ml, he failed to respond with a normal rise in titer after immunization with ‘A' and ‘B' blood group substances, diphtheria, tetanus, or Types I and II poliovaccines. When the total immunoglobulin level in the youngest boy was 1564 mg/100 ml, he had absent ‘B' and low ‘A' isohemagglutinins. Later studies showed that he failed to respond with a normal rise in titer after stimulation with ‘A' and ‘B' blood group substances, diphtheria, tetanus, typhoid, and Types I, II and III poliovaccines. Similar studies in family members demonstrated a marked polyclonal IgA hyperglobulinemia and specific immunologic unresponsiveness to ‘B' substance in the mother (tables I and II). She also gave poor circulating antibody responses to immunization with diphtheria and poliovaccines. Two maternal aunts had high normal levels of IgA and low isohemagglutinin titers (table VII). We are unaware of other reports of specific immunologic unresponsiveness and/or antibody deficiency in the apparent heterozygote for what appears to be an X-linked immunologic deficiency. A male maternal first cousin also had a high normal level of IgA, asthma, shortness of stature and repeated respiratory infections. These findings provide direct evidence for a genetic influence in some forms of acquired immunologic deficiency. Speculation: The heterogeneity of immunologic abnormality observed in this family is inconsistent with many of the current hypotheses of the genetic defects in immunologic deficiency. An afferent phase defect seems to offer the best explanation for a single genetic mechanism of immunologic deficiency in this family. The question of a possible contributory role of repeated bacterial infections in the apparent progression and heterogeneity of immunologic deficiency in the members of this sibship is raised.

Intestinal lymphangiectasia: a protein-losing enteropathy with hypogammaglobulinemia, lymphocytopenia and impaired homograft rejection.

Intestinal lymphangiectasia is a disease characterized by dilated intestinal lymphatics, protein-losing enteropathy, hypoalbuminemia, and edema. The immunologic status of 18 patients with intestinal lymphangiectasia was studied. Concentrations of IgG, IgA, and IgM were measured by immune precipitation and metabolism of these three immunoglobulins was studied using purified radioiodinated proteins. The serum concentration and total body pool of each immunoglobin were greatly reduced. The fraction of the intravascular protein pool catabolized per day was increased to 34% for IgG, 59% for IgA, and 66% for IgM; these are in contrast with control values of 7%, 28%, and 17%, respectively. Synthetic rates of the immunoglobulins were normal or slightly increased. Primary circulating antibody response was tested in five patients with Vi and tularemia antigens. Titers elicited in patients with the Vi antigen were significantly lower than those seen in a control group, whereas no difference was seen between patient and control responses to the tularemia antigen. Lymphocytopenia was noted in patients with intestinal lymphangiectasia. The mean circulating lymphocyte count was 710 +/- 340/mm(3) in contrast to 2500 +/- 600/mm(3) in controls. Cellular hypersensitivity was studied with skin tests and skin grafts. 91% of normal individuals reacted to at least one of the four skin test antigens: purified protein derivative, mumps, Trichophyton, and Candida albicans; in contrast, only 17% of patients with intestinal lymphangiectasia had a positive reaction. Each of three patients tested with dinitrochlorobenzene had a negative reaction. Finally, all four patients who received skin homografts have retained these grafts for at least 12 months. The immunological disorders in patients with intestinal lymphangiectasia appear to result from loss of immunoglobulins and lymphocytes into the gastrointestinal tract secondary to disorders of lymphatic channels. Lymphocyte depletion then leads to skin anergy and impaired homograft rejection.

Immunologic Studies in Lichen Myxedematosus

A patient with lichen myxedematosus of 13 years' duration has experienced stabilization or regression of the disease. The long duration of clinical well-being suggests that this patient is not suffering from a variant of multiple myeloma. Serum protein studies reveal an abnormal serum protein in the γ-globulin region. Immunoglobulin IgA levels in serum are abnormally high. Circulating antibody responses after immunization with Vi and brucellin antigens and delayed hypersensitivity responses in this patient are apparently normal.

Immediate Hypersensitivity Reactions Induced in Mice by Active and Passive Means

Summary Immediate hypersensitivity of the Arthus type was produced in mice sensitized actively or passively. The most successful procedure of producing strong hypersensitivity to hen's egg albumin (HEA) was by subcutaneous injection of 0.5 to 1 mg in Freund's adjuvant, either containing or lacking mycobacteria, and then skin testing them successively on the 20th, 25th and 30th days thereafter. Almost 100% of the mice react strongly during the second and third skin test. The circulating antibody response showed that whenever skin test reactions are observed, circulating antibodies are present and that skin test with as little as 0.8 µg of HEA produced a noticeable increase in circulating antibody titers as well as enhancement of skin sensitivity. The Arthus reactions produced by transferring hyperimmune mouse serum to mice were similar to those produced in actively sensitized animals. It required at least 250 µg of mouse anti-HEA antibody nitrogen given intraperitoneally to produce skin sensitivity. As much as 1000 µg of AbN of a rabbit anti-HEA serum failed to produce visible skin sensitization. Histologic studies of the skin reactions showed that the predominant cell type infiltrating the reaction site was the polymorphonuclear leukocyte. Only in those mice sensitized with HEA in complete Freund's adjuvant were there, at 24 to 48 hr after skin test, a few areas with mononuclear cells present. It was concluded that the reactions observed were of the Arthus type and that the 24-hr reactions observed were residual Arthus reactions. No true delayed hypersensitivity to HEA was observed.

Lymphoid tissue abnormalities associated with ataxia-telangiectasia

Systematic morphologic and functional studies of the immune system were undertaken in eight patients with ataxia-telangiectasia. Seven of the eight had siblings with the disease. Three died, one apparently of pneumonia, one of pneumococcal meningitis and one of small cell lymphosarcoma. No thymus was found at autopsy in one; in another, the thymus was small, lacking in Hassall's corpuscles and embryonic in appearance. Two thymus biopsy specimens in other patients had this same histologic abnormality. Lymph nodes were normal in two instances, abnormal in six; and tonsillar tissue was deficient in follicle formation in all four patients in whom biopsy was performed. As a group, these patients tended to have hematologic abnormalities involving elements other than lymphoid cells; but these were quite variable, both in the cell lines involved and the degree of deficit or hyperplasia.All the patients had an immunologic deficit, observed most consistently in the response to skin homografts and antigens ordinarily provocative of delayed allergic responses. The circulating antibody response to certain antigens was also deficient in most of the children.These additional data on our patient group, and those from other published reports, emphasize the association of this neurologic and vascular disease with defective thymic development, generalized lymphoreticular abnormalities, immunologic deficiency (particularly of cellular immunity), and unusual susceptibility to lymphoreticular malignancy.

ATAXIA TELANGIECTASIA WITH CEREBELLAR TUMOR

Two patients with ataxia telangiectasia were studied. There is absence of γA immunoglobulin, poor delayed hypersensitivity skin reactions, and abnormal rejection of skin grafts. The susceptibility to sinopulmonary infections is probably related to the abnormal cellular and circulating antibody responses which these patients demonstrate. Experimental evidence indicates that the fundamental immunologic defect in this disease lies in thymus gland. The etiology of the neurologic abnormalities is unknown. The first instance of a cerebellar tumor to develop in this syndrome is reported.

Observations on Circulating Antibody Responses to Mycobacterial Stimuli

Observations on Circulating Antibody Responses to Mycobacterial Stimuli

INFECTION AND IMMUNITY IN CHRONIC LYMPHOCYTIC LEUKEMIA

Shaw and co-workers¹present a study of the immunologic response of patients with chronic lymphocytic leukemia to bacterial infection. In their experience the absolute granulocyte counts, the polymorphonuclear response to infection, and the phagocytic function of the polymorphonuclear cells were found to be normal in these patients. However, a decreased or even absent circulating antibody response to antigenic stimulation was observed. These findings pointed to a failure of the immunologic response. In a group of 18 patients with chronic lymphocytic leukemia admitted to the Clinical Center at Bethesda, Md., 10 patients, according to Shaw, had multiple bacterial infections and five of these died. Hypogammaglobulinemia in this group appeared to be directly related to the incidence and severity of these infections. A study of the serum γ-globulin concentrations and circulating antibody production was undertaken with regard to bacterial infection. In a later group of 42 patients with chronic lymphocytic leukemia