Development of Functional Antibodies Directed to Human Dialyzable Leukocyte Extract (Transferon®).

Transferon® is an immunomodulator made of a complex mixture of peptides from human dialyzable leucocyte extracts (hDLEs). Development of surrogate antibodies directed to hDLE is an indispensable tool for studies during process control and preclinical trials. These antibodies are fundamental for different analytical approaches, such as identity test and drug quantitation, as well as to characterize its pharmacokinetic and mechanisms of action. A previous murine study showed the inability of the peptides of Transferon® to induce antibody production by themselves; therefore, in this work, two approaches were tested to increase its immunogenicity: chemical conjugation of the peptides of Transferon® to carrier proteins and the use of a rabbit model. Bioconjugates were generated with Keyhole Limpet Hemocyanin (KLH) or Bovine Serum Albumin (BSA) through maleimide-activated carrier proteins. BALB/c mice and New Zealand rabbits were immunized with Transferon® conjugated to KLH or nonconjugated Transferon®. Animals that were immunized with conjugated Transferon® showed significant production of antibodies as evinced by the recognition of Transferon®-BSA conjugate in ELISA assays. Moreover, rabbits showed higher antibody titers when compared with mice. Neither mouse nor rabbits developed antibodies when immunized with nonconjugated Transferon®. Interestingly, rabbit antibodies were able to partially block IL-2 production in Jurkat cells after costimulation with Transferon®. In conclusion, it is feasible to elicit specific and functional antibodies anti-hDLE with different potential uses during the life cycle of the product.

Preparation and identification of transfer factor specific to Staphylococcus aureus in vitro.

The objective of the study was to explore the methods for preparing transfer factor specific to Staphylococcus aureus (SA-STF) in vitro. Under the optimum conditions, the spleen cells of rabbits were immunized with SA in vitro to prepare SA-STF, and the immune activities were identified with the phagocytosis and sterilization, skin delayed-type hypersensitivity, and immune protection tests. The concentration of polypeptide was 2.26 ± 0.27 mg/mL, and ribose was 0.684 ± 0.094 mg/mL. The phagocytosis and sterilization rates of the STF group were 70.9 ± 12.4% and 62.1 ± 12.2%, respectively, and compared with the non-specific transfer factor (NTF) group, there were no significant differences (P = 0.074 and 0.069, respectively). The skin was inflamed and marked nodules formed at the injection site in the mice of the STF group rather than the NTF and control groups. The survival rate of the STF-1 group was significantly higher than the survival rates of the STF-2 (P = 0.024) and NTF groups (P = 0.016). SA-STF was prepared and characterized successfully in vitro, and it probably is a biological candidate for therapy or adjuvant therapy for diseases caused by Staphylococcus aureus.

Eventos adversos observados años después del tratamiento con factor de transferencia / Adverse events occurred some years after the application of a transfer factor treatment

Introducción: el factor de transferencia es un inmunoestimulante que se emplea en varias enfermedades, su seguridad en las condiciones de la práctica médica no se ha establecido. Objetivos: identificar eventos adversos presentados años después de finalizado el tratamiento con factor de transferencia y determinar la relación entre su utilización y los eventos observados. Métodos: estudio observacional, retrospectivo, de fármacovigilancia activa. El universo estuvo constituido por 413 pacientes tratados con este fármaco entre los años 2001 y 2004 en 11 hospitales de La Habana. El periodo de observación abarcó los 6 a 8 años posteriores al tratamiento. Los pacientes fueron entrevistados acerca de la presencia de infecciones, cáncer y otros eventos, en su hogar. Si un evento era la muerte, se entrevistaba al familiar para registrar causa y fecha. Resultados: se entrevistaron 356 pacientes, 66 (18,53 por ciento) presentaron al menos un evento adverso, 21(31,8 por ciento) en mayores de 60 años. Se registraron 87 eventos adversos, 8 (9,2 por ciento) fueron infecciones como hepatitis B, hepatitis C, foliculosis, mononucleosis y verrugas vulgares, 1 (1,1 por ciento) cáncer y 78 (89,7 por ciento) otros eventos. Su relación con la administración del fármaco resultó condicional en 64 (73,6 por ciento) pacientes e improbable en 21 (24,1 por ciento), en esta última categoría se incluyeron las infecciones y la mayoría de los eventos mortales. Conclusiones: los eventos adversos que se registraron en los pacientes, años después de haber recibido tratamiento con factor de transferencia, no se consideran relacionados con su administración, aunque necesitan ser vigilados pues la información obtenida en este estudio debe ser contrastada con un mayor número de observaciones y estudios observacionales controlados

Introduction: the transfer factor is an immunostimulant that is used to treat several diseases but its safety in the medical practice has not been assured yet. Objectives: to identify the adverse events occurred some years after the end of a transfer factor treatment and to determine the association of the use and the observed events. Methods: observational active drug surveillance study. The universe of study was 413 patients who were treated with the transfer factor from 2001 to 2004 in eleven hospitals located in La Habana province. The observation period ranged 6 to 8 years after the treatment. The patients were interviewed at home on the occurrence of infections, cancer or any other events. If some death occurred, then a family member was interviewed to record the cause and the date of the decease. Results: three hundred fifty six patients were interviewed; 66(18.53 percent) stated at least one adverse event and 21(31.80 percent) events occurred in over 60 years-old patients. Eighty seven adverse effects were recorded; 8 (9.20 percent) comprised infections such as hepatitis B, hepatitis C, foliculosis, mononucleosis and warts, one (1.10 percent) event corresponded to cancer and 78 (89.70 percent) to other type of events. Their relationship with the administration of the drug was considered as conditional in 64 events (73.60 percent) and as unlikely in 21 (24.10 percent) events comprising infections and most of the fatal events. Conclusions: the adverse events observed in the patients, some years after the end of the treatment with the transfer factor, were not considered to be related to the administration of this drug; however, they must be under surveillance since the information obtained from this study should be compared with the information collected by a higher number of observations and of controlled observational studies

Eventos adversos observados años después del tratamiento con factor de transferencia / Adverse events occurred some years after the application of a transfer factor treatment

Introducción: el factor de transferencia es un inmunoestimulante que se emplea en varias enfermedades, su seguridad en las condiciones de la práctica médica no se ha establecido. Objetivos: identificar eventos adversos presentados años después de finalizado el tratamiento con factor de transferencia y determinar la relación entre su utilización y los eventos observados. Métodos: estudio observacional, retrospectivo, de fármacovigilancia activa. El universo estuvo constituido por 413 pacientes tratados con este fármaco entre los años 2001 y 2004 en 11 hospitales de La Habana. El periodo de observación abarcó los 6 a 8 años posteriores al tratamiento. Los pacientes fueron entrevistados acerca de la presencia de infecciones, cáncer y otros eventos, en su hogar. Si un evento era la muerte, se entrevistaba al familiar para registrar causa y fecha. Resultados: se entrevistaron 356 pacientes, 66 (18,53 por ciento) presentaron al menos un evento adverso, 21(31,8 por ciento) en mayores de 60 años. Se registraron 87 eventos adversos, 8 (9,2 por ciento) fueron infecciones como hepatitis B, hepatitis C, foliculosis, mononucleosis y verrugas vulgares, 1 (1,1 por ciento) cáncer y 78 (89,7 por ciento) otros eventos. Su relación con la administración del fármaco resultó condicional en 64 (73,6 por ciento) pacientes e improbable en 21 (24,1 por ciento), en esta última categoría se incluyeron las infecciones y la mayoría de los eventos mortales. Conclusiones: los eventos adversos que se registraron en los pacientes, años después de haber recibido tratamiento con factor de transferencia, no se consideran relacionados con su administración, aunque necesitan ser vigilados pues la información obtenida en este estudio debe ser contrastada con un mayor número de observaciones y estudios observacionales controlados(AU)

Introduction: the transfer factor is an immunostimulant that is used to treat several diseases but its safety in the medical practice has not been assured yet. Objectives: to identify the adverse events occurred some years after the end of a transfer factor treatment and to determine the association of the use and the observed events. Methods: observational active drug surveillance study. The universe of study was 413 patients who were treated with the transfer factor from 2001 to 2004 in eleven hospitals located in La Habana province. The observation period ranged 6 to 8 years after the treatment. The patients were interviewed at home on the occurrence of infections, cancer or any other events. If some death occurred, then a family member was interviewed to record the cause and the date of the decease. Results: three hundred fifty six patients were interviewed; 66(18.53 percent) stated at least one adverse event and 21(31.80 percent) events occurred in over 60 years-old patients. Eighty seven adverse effects were recorded; 8 (9.20 percent) comprised infections such as hepatitis B, hepatitis C, foliculosis, mononucleosis and warts, one (1.10 percent) event corresponded to cancer and 78 (89.70 percent) to other type of events. Their relationship with the administration of the drug was considered as conditional in 64 events (73.60 percent) and as unlikely in 21 (24.10 percent) events comprising infections and most of the fatal events. Conclusions: the adverse events observed in the patients, some years after the end of the treatment with the transfer factor, were not considered to be related to the administration of this drug; however, they must be under surveillance since the information obtained from this study should be compared with the information collected by a higher number of observations and of controlled observational studies(AU)

Eventos adversos observados después del tratamiento con factor de transferencia / Adverse events after treatment with the transfer factor

Introducción: el factor de transferencia es un inmunoestimulante que se emplea en una amplia gama de enfermedades. Su eficacia y seguridad han sido evaluadas en ensayos clínicos prerregistro, pero se conoce poco sobre su seguridad en condiciones de la práctica habitual, de ahí la necesidad de vigilar su uso y contribuir a establecer su relación beneficio/riesgo. Objetivos: identificar eventos adversos en pacientes tratados con factor de transferencia, determinar grado de asociación fármaco-evento observado y su gravedad. Métodos: estudio observacional, descriptivo, prospectivo y multicéntrico de farmacovigilancia activa. Se observó durante el año siguiente al término del tratamiento con factor de transferencia, a una serie de 282 pacientes tratados por su médico de asistencia entre abril de 2001 y abril de 2002, en 9 hospitales en La Habana. Se analizaron los eventos adversos presentados, su gravedad, si existía asociación con el fármaco, la cantidad de eventos por paciente, la dosis administrada y la edad del paciente. Resultados: el 13,8 por ciento de los pacientes observados tuvo al menos un evento adverso, de ellos 38,5 por ciento tenía entre 45-59 años. Los esquemas de tratamiento con dosis altas y prolongadas no provocaron más eventos que los ya encontrados. Se identificaron 80 eventos adversos, 55 por ciento leves y en 80 por ciento se consideró improbable su relación con el medicamento. Ninguno se clasificó definitivo o probable, mientras que eventos como fiebre, artralgia, disnea, mialgia, alergia y astenia, se consideraron reacciones adversas posibles y leves. Conclusiones: la mayoría de los eventos adversos presentados, durante el año siguiente de finalizado el tratamiento con factor de transferencia, fueron leves y no relacionados con su uso. Aun así, los productores del medicamento deberían advertir a profesionales y pacientes sobre las reacciones adversas posibles detectadas

Introduction: the transfer factor is an immunologic stimulant used in a wide range of diseases. Its safety and efficiency have been evaluated in pre-registration clinical trials, but little is known about its safety margin under regular practical conditions, hence the need of closely watching its use and setting the benefit-risk relation. Objectives: to identify adverse events in patients treated with the transfer factor and to determine the level of association of the drug and the observed adverse event and severity. Methods: prospective, multicentered, descriptive and observational study of active drug surveillance. Two hundred and eighty two patients, who were attended by their physicians from April 2001 to April 2002 in 9 hospitals of Havana, were observed for one year after the end of a treatment with the transfer factor. The occurrence of adverse events as well as their severity, association with the drug, the number of events per patient, the supplied dosage and the age of the patient was all analyzed. Results: in this group of patients, 13,8 percent had at least one adverse effect; 38,5 percent were aged 45 to 59 years. The treatment schemes with high and prolonged dosage did not cause any further event. Eighty adverse effects were identified, 55 percent mild and 80 percent were considered as unlikely related with the drug. None of them was definitive or probable whereas fever, arthralgia, dysnea, myalgia, allergy and asthenia were considered as possible mild adverse reactions. Conclusions: most of adverse events during the year after the end of treatment with the transfer factor were mild and unrelated to the use of the drug. However, the drug manufacturers should advise professionals and patients on the possible occurrence of adverse reactions

Eventos adversos observados después del tratamiento con factor de transferencia / Adverse events after treatment with the transfer factor

Introducción: el factor de transferencia es un inmunoestimulante que se emplea en una amplia gama de enfermedades. Su eficacia y seguridad han sido evaluadas en ensayos clínicos prerregistro, pero se conoce poco sobre su seguridad en condiciones de la práctica habitual, de ahí la necesidad de vigilar su uso y contribuir a establecer su relación beneficio/riesgo. Objetivos: identificar eventos adversos en pacientes tratados con factor de transferencia, determinar grado de asociación fármaco-evento observado y su gravedad. Métodos: estudio observacional, descriptivo, prospectivo y multicéntrico de farmacovigilancia activa. Se observó durante el año siguiente al término del tratamiento con factor de transferencia, a una serie de 282 pacientes tratados por su médico de asistencia entre abril de 2001 y abril de 2002, en 9 hospitales en La Habana. Se analizaron los eventos adversos presentados, su gravedad, si existía asociación con el fármaco, la cantidad de eventos por paciente, la dosis administrada y la edad del paciente. Resultados: el 13,8 por ciento de los pacientes observados tuvo al menos un evento adverso, de ellos 38,5 por ciento tenía entre 45-59 años. Los esquemas de tratamiento con dosis altas y prolongadas no provocaron más eventos que los ya encontrados. Se identificaron 80 eventos adversos, 55 por ciento leves y en 80 por ciento se consideró improbable su relación con el medicamento. Ninguno se clasificó definitivo o probable, mientras que eventos como fiebre, artralgia, disnea, mialgia, alergia y astenia, se consideraron reacciones adversas posibles y leves. Conclusiones: la mayoría de los eventos adversos presentados, durante el año siguiente de finalizado el tratamiento con factor de transferencia, fueron leves y no relacionados con su uso. Aun así, los productores del medicamento deberían advertir a profesionales y pacientes sobre las reacciones adversas posibles detectadas(AU)

Introduction: the transfer factor is an immunologic stimulant used in a wide range of diseases. Its safety and efficiency have been evaluated in pre-registration clinical trials, but little is known about its safety margin under regular practical conditions, hence the need of closely watching its use and setting the benefit-risk relation. Objectives: to identify adverse events in patients treated with the transfer factor and to determine the level of association of the drug and the observed adverse event and severity. Methods: prospective, multicentered, descriptive and observational study of active drug surveillance. Two hundred and eighty two patients, who were attended by their physicians from April 2001 to April 2002 in 9 hospitals of Havana, were observed for one year after the end of a treatment with the transfer factor. The occurrence of adverse events as well as their severity, association with the drug, the number of events per patient, the supplied dosage and the age of the patient was all analyzed. Results: in this group of patients, 13,8 percent had at least one adverse effect; 38,5 percent were aged 45 to 59 years. The treatment schemes with high and prolonged dosage did not cause any further event. Eighty adverse effects were identified, 55 percent mild and 80 percent were considered as unlikely related with the drug. None of them was definitive or probable whereas fever, arthralgia, dysnea, myalgia, allergy and asthenia were considered as possible mild adverse reactions. Conclusions: most of adverse events during the year after the end of treatment with the transfer factor were mild and unrelated to the use of the drug. However, the drug manufacturers should advise professionals and patients on the possible occurrence of adverse reactions(AU)

Preparation and properties of the specific anti-influenza virus transfer factor.

Specific anti-influenza virus and normal transfer factors prepared in an experimental animal model, the pig, have been tested for their components, characteristics, and activity of known specificity. Two transfer factors are small molecular mixture which consist entirely or partly of polypeptides and polynucleosides. Moreover, the biological activity of transfer factors could be approved by Rosettes test and specific skin test. The study would lay a foundation for the research and development of other specific transfer factor.

Efectos adversos asociados al tratamiento con factor de transferencia: ciudad de La Habana, 2004 / Adverse drug effects associated to the treatment of patients with transfer factor. City of Havana, 2004

El factor de transferencia (Hebertrans) constituye un inmunoestimulante que se emplea en una amplia gama de enfermedades. Su seguridad ha sido evaluada en los ensayos clínicos pre-registro, pero no así en investigaciones poscomercialización, por tal motivo se realizó un estudio observacional y multicéntrico de vigilancia activa, en pacientes tratados con factor de transferencia en 11 hospitales de la Ciudad de La Habana , para identificar los eventos presentados durante el tratamiento, así como clasificarlos según su causalidad y gravedad. La información fue recogida por el médico inmunólogo de cada hospital y supervisada por el farmacoepidemiólogo hospitalario. Durante el tratamiento se obtuvo información de 387 pacientes y se reportaron 133 eventos en 86 casos (22,2 por ciento). Los más frecuentes fueron fiebre, dolor y eritema en el sitio de la inyección, cefalea y diarrea; el 92,5 por ciento de los eventos observados fueron leves. El 27,8 por ciento se clasificó como definitivamente provocados por el fármaco, estos últimos relacionados con la vía de administración. El factor de transferencia resultó un medicamento seguro en los pacientes observados(AU)

[Inflammatory mediators in patients with atopic dermatitis after treatment with transfer factor]. / Mediadores inflamatorios en pacientes con dermatitis atópica posterior al tratamiento con factor de transferencia.

BACKGROUND: Atopic dermatitis is a skin inflammatory disease, which is associated to high levels of IgE, eosinophiles and change of T lymphocytes. OBJECTIVE: To determine if the treatment with transfer factor for moderate atopic dermatitis decreases the number of inflammatory cells in the peripheral blood. MATERIAL AND METHODS: We selected twenty patients with diagnosis of moderate atopic dermatitis. The age range of the patients was between 5 and 45 years old. Patients were assigned to one of three groups: group A included patients with atopic dermatitis treated with transfer factor: one unit a day for five days, two units a week, one unit a week, one unit every fifteen days and one unit a month. Group B included ten patients with atopic dermatitis who received conventional treatment (hydroxyzine 10 mg/24 h) and the group C was conformed by healthy controls. All patients were submitted to basal and final determination of IgE, peripheral blood eosinophils, and underpopulation of lymphocytes by flow cytometry. Study period was of ten weeks. RESULTS: Levels of IgE were reduced respect to the basal value. In the patients of group A there was an increase in neutrophils and leukocytes after treatment; however, it was not significant (p = 0.46). Eosinophils were significantly reduced (p = 0.01). After comparing group A to group C the p value was of 0.035. CONCLUSION: In patients with atopic dermatitis, after 10 weeks of treatment with transfer factor, the level of IgE and peripheral eosinophils was reduced.

Transfer factor as an adjuvant to non-small cell lung cancer (NSCLC) therapy.

The rationale for using transfer factor (TF) in lung cancer patients is that the possibility of improving their cell-mediated immunity to tumour associated antigens (TAA) may improve their survival. From Jan 1984 to Jan 1995, 99 non-small cell lung cancer (NSCLC) resected patients were monthly treated with TF, extracted from the lymphocytes of blood bank donors. In the same period, 257 NSCLC resected patients were considered as non-treated controls. The survival rates of the TF treated group appear significantly improved both for patients in stages 3a and 3b, and patients with histological subtype "large cell carcinoma" (P < 0.02). Survival of TF treated patients is also significantly higher (P < 0.02) for patients with lymph node involvement (N2 disease). The results of this study suggest that the administration of TF to NSCLC resected patients may improve survival.

[Treatment of extrinsic bronchial asthma with transfer factor]. / Tratamiento del asma bronquial extrínseca con factor de trasferencia.

A group of 90 external asthmatics with cellular immunodeficiency or not was studied and treated during 10 months with transfer factor or double blind placebo. Total immunoglobulin serum studies (A, G, M and E), spontaneous rosette and intradermal tests, were made a month before the treatment's beginning and a month after the ending of the treatment. The patients were clinically evaluated every day in accordance to the intensity and the frequency of their crisis and with the immunological point of view of the tests made. There was not significant differences between the study groups treated with the transfer factor or not. Adverse reactions were not noticed.

Effect of transfer factor on myelosuppression and related morbidity induced by chemotherapy in acute leukaemias.

The aim of this study is to determine the safety and efficacy of Transfer Factor (TF) in accelerating the haematopoietic recovery in patients with acute leukaemias (AL), following intensive therapy to induce remission of the disease. Twenty-two patients with different types of AL (16 AML, three BC-CML and three ALL) were studied. The patients were divided in two groups. Group 1 (eight AML, two BC-CML and one ALL) received, after myelosuppression induced by chemotherapy, TF (1 unit daily, subcutaneous) until leucocyte count was > 2.5 x 10(9)/l and platelet count > 80 x 10(9)/l. Group 2 was considered the control group and did not receive TF. Treatment with TF accelerated the recovery of neutrophils, leucocytes, platelets (P < 0.001) and haemoglobin (P < 0.01). As a logical consequence, incidence and severity of infection and haemorrhage were lesser in the TF group than in the control group. There was no evidence that TF accelerated the re-growth of leukaemic cells. It seems that TF is safe in AL, accelerating haematopoietic recovery. However, it should be used with caution until results of additional trials become available.

An outbreak of viral hepatitis B associated with transfer factor administration.

An outbreak of viral hepatitis B in patients of the allergological clinic of the teaching hospital in Olomouc in connection with application of the crude non ultrafiltrated transfer factor is described. The epidemic was the first one of this kind observed in Czechoslovakia in connection with this blood derivative. A total of 32 persons from 13 districts in Czechoslovakia fell ill, yet thanks to close cooperation of epidemiologists of many districts and regions of Czechoslovakia the epidemic was brought under control in its full extent.

Failure of transfer factor therapy in atopic dermatitis.

A controlled clinical study was conducted on 6 patients with atopic dermatitis to assess the efficacy of transfer factor. After the code was broken the 3 patients treated with placebo preparation were treated with transfer factor for a further period of 10 weeks. No definite therapeutic effects could be demonstrated. The immunological in vivo and in vitro tests failed to reveal any effects except for a change to positive in the tuberculin skin test in those patients who had previously been skin test negative. The treatment had to be discontinued in one patient due to a suspected allergic reaction against transfer factor.

[Transfer factor. Properties and possible therapeutic applications (author's transl)]. / Transferfaktor. Eigenschaften und therapeutische Anwendungsmöglichkeiten

Transfer factor (TF) is a dialysable and ultrafilterable extract from human leukocytes. It contains only substances with a molecular weight of less than 10 000. Several biological activities of TF are so far known. These refer to the transfer of specific cellular immunity from one individual to another and a stimulating effect, probably of an unspecific nature, on the cellular immune system. So far, favorable therapeutic results have been obtained in chronic candidiasis and a few other chronic infectious diseases, in the Wiskott-Aldrich syndrome and possibly also in some special malignant tumors. The small number of treatments does not permit any firm conclusions to be drawn.