Macrophage-derived human resistin is induced in multiple helminth infections and promotes inflammatory monocytes and increased parasite burden.

Parasitic helminth infections can be associated with lifelong morbidity such as immune-mediated organ failure. A better understanding of the host immune response to helminths could provide new avenues to promote parasite clearance and/or alleviate infection-associated morbidity. Murine resistin-like molecules (RELM) exhibit pleiotropic functions following helminth infection including modulating the host immune response; however, the relevance of human RELM proteins in helminth infection is unknown. To examine the function of human resistin (hResistin), we utilized transgenic mice expressing the human resistin gene (hRetnTg+). Following infection with the helminth Nippostrongylus brasiliensis (Nb), hResistin expression was significantly upregulated in infected tissue. Compared to control hRetnTg- mice, hRetnTg+ mice suffered from exacerbated Nb-induced inflammation characterized by weight loss and increased infiltration of inflammatory monocytes in the lung, along with elevated Nb egg burdens and delayed parasite expulsion. Genome-wide transcriptional profiling of the infected tissue revealed that hResistin promoted expression of proinflammatory cytokines and genes downstream of toll-like receptor signaling. Moreover, hResistin preferentially bound lung monocytes, and exogenous treatment of mice with recombinant hResistin promoted monocyte recruitment and proinflammatory cytokine expression. In human studies, increased serum resistin was associated with higher parasite load in individuals infected with soil-transmitted helminths or filarial nematode Wuchereria bancrofti, and was positively correlated with proinflammatory cytokines. Together, these studies identify human resistin as a detrimental factor induced by multiple helminth infections, where it promotes proinflammatory cytokines and impedes parasite clearance. Targeting the resistin/proinflammatory cytokine immune axis may provide new diagnostic or treatment strategies for helminth infection and associated immune-mediated pathology

Mieloma múltiple extra-óseo, un caso con mala evolución ¿es lo usual?

PB-021 Introducción: El mieloma extramedular (MEM) se presenta al diagnóstico en 3-18% de los casos y otro 10-30% lo padecerá en algún en la evolución. Esta presentación de MM se asocia a morfología inmadura, Cg de alto riesgo, escape de cadenas ligeras, disminución en la expresión de CD56y aumento en la expresión de CD44 y CXCR4; con peor pronóstico pese a los avances en el tratamiento. Metodologia: Presentamos el caso de un paciente con diagnóstico de MM IgA K extra óseo con una evolución desfavorable. Diagnóstico inicial en Febrero 2014 ISS I, con plasmocitoma en V, VIII y IX arco costal, recibió tratamiento con VD por 6 ciclos alcanzando RC y posteriormente TASPE y consolidación con Velcade por 6 ciclos. Primer recaída en Ago 2016 con masa en pared torácica sin contacto óseo; escape a CLL K, tratamiento con VRD por 6 ciclos logrando RC y segundo TASPE y mantenimiento con R. Segunda recaída en Mayo 2018 con derrame pleural y ascitis maligna, tratamiento con DVd por 1 ciclo y progresión intratratamiento; cambio a Pomalidomida-Claritromicina- Dexametasona sin respuesta, desarrollo de insuficiencia respiratoria, fallo renal y hepático culminando en su fallecimiento en Agosto 2018. Conclusiones: Acorde a lo reportado, la supervivencia de la paciente fue menor a lo esperado por escalas de riesgo (ER) habitual (ISS) y el grado de respuesta alcanzado con el tratamiento, la SG fue de 54 meses con SLP 31 meses, la supervivencia después de la segunda recaída fue de 3 meses, similar a lo ya descrito (6 meses). Acorde a un estudio realizado por Weinstock el MEM solo 1, 32% de los MEM se manifestaron con enfermedad pleural y derrame, y 0, 62% en peritoneo y ascitis (como en el caso). Al igual que lo reportado, la enfermedad de la paciente presentó liberación de cadenas ligeras. Si bien existe evidencia y ..

Avisalmvac: evaluation studies of stability and toxicity

In Pasteur Institute laboratories there was developed AVISALMVAC, a vaccine against avian Salmonella, a biological product that contains S. enteritidis and S. typhimurium bacterin, with oil adjuvant. This paper presents the results of the studies regarding the stability and toxicity evaluation of this vaccine stored under conditions recommended by the manufacturer (2-80C) at the end of the period of validity. The vaccine stability was assessed by serological and histopathological analysis of samples from SPF chickens vaccinated with the product at the end of the period of validity. The study of Avisalmvac toxicity was carried out by inoculation of the product or its components on Vero cell monolayer, and the effects were microscopically recorded or by MTT test, applied at 6 days post-inoculation. Antibody titers recorded at 2 and 3 weeks post vaccination demonstrated the vaccine ability (used after an year since manufacture) to induce synthesis of specific antibodies and therefore, the product stability was proven. Histopathological examinations carried out on samples taken at 18 days post vaccinationfrom the vaccination site (skeletal muscle and skin) and spleen, did not show any lesions associated to vaccination with Avisalmvac. The cytotoxicity analysis made by inoculating the vaccine or its components on Vero cell monolayer and the microscopic examination did not record visible cytopathic effects for any vaccine dilutions or vaccine components. The cell metabolism evaluation by MTT assay made at 6 days after vaccine/vaccine components inoculation on Vero monolayer, shown the ability of the vaccine and oil adjuvant to stimulate cell metabolism, and a certain degree of toxicity / inhibition of dehydrogenase metabolism associated to one of emulsifier but at dilutions higher than those used in the vaccine formula

Polymorphism of IL-1alpha, IL-1beta and IL-10 in patients with advanced ovarian cancer: Results of a prospective study with 147 patients

OBJECTIVE.: Interleukin 1 (IL-1) and IL-10 are critically involved in tumorigenesis. We investigated polymorphisms of IL-1 and IL-10 genes in patients with ovarian cancer (OC). METHODS.: In a prospective, case-control study 147 patients with OC and 129 patients without history of any malignancy (CG) were genotyped for IL-1 gene (IL-1alpha -889 T/C and IL-1beta -511 C/T) and IL-10 gene (IL-10 -1082 G/A, -819 C/T and -592 C/A) using pyrosequencing. RESULTS.: IL-10 polymorphisms in -819 and -592 positions correlated with the postoperative residual tumor mass (p=0.036 and p=0.035, respectively). The chance of achieving optimal tumor debulking was 1.49 times greater for patients with the C/C genotype at -819 and -512 positions than for patients with other genotypes. There were no significant associations between allelic frequencies for IL-1alpha and IL-1beta in OC. IL-10 -819 CC and -592 CC genotypes were associated in univariate analysis with a better disease-free and overall survival. CONCLUSIONS.: IL-10 promoter polymorphism may be related with the ability to achieve optimal tumor debulking. Polymorphism in IL-10 gene seems to influence the overall and disease-free survival rate. Subsequent multi-institutional studies with high number of patients are warranted to confirm these results