Ambiente e Salute News n.11 - settembre-ottobre 2021

Less is more: measuring body temperature during well child visits is not good for the child A recent retrospective study found the risk of prescribing unnecessary tests and therapies to the child in case of routine fever measurement during the well child visit. The article of the month discusses the need to offer clinical pathways based on evidence-based medicine.

P1381SWITCHING FROM IRON GLUCONATE TO FERRIC CARBOXYMALTOSE CAN BE ASSOCIATED WITH A BETTER CONTROL OF IRON STATUS AND ANEMIA IN HEMODIALYSIS PATIENTS?

Background and Aims Before evaluating any ESA treatment, International guidelines (NICE-2015, KDIGO-2012, ERBP–2013) suggest to administer iron first to patients with iron deficiency anemia and not still on ESA therapy. Moreover anemic CKD patients treated with ESA should be iron supplemented (unless ferritin is> 800 mcg/l) to maximize the benefits of ESAs. A recent retrospective study of switching iron sucrose to ferric carboxymaltose (FCM), conducted by Hofman et al., showed a better control of iron status in hemodialysis (HD) patients. New generation drugs, like carboxymaltose, may change the iron administration methods on dialysis, due to their different properties: therefore more experience is needed. In the following evaluation we report the results of switching from iron gluconate (our previous standard therapy) to FCM in HD patients. Primary Endpoint switching effects on iron parameters (TSAT, ferritin) and hemoglobin. Secondary Endpoints switching effects on iron and ESA doses administered Method Study design: retrospective review of data from 106 HD patients from 2 Italian different dialysis centers, who were switched from iron gluconate to ferric carboxymaltose in a 1: 1 ratio. Study duration: 9 months (3 months pre-switch, 6 months post-switch) Treatment schedule: -ferritin <100 ng/ml and/or TSAT <20%: 100 mg of iron/weekly -ferritin <200 μg/l, or TSAT<20%: 100 mg of iron/weekly -ferritin 200–500 μg/l, and/or TSAT 20–30%: 100 mg of iron/every 2 weeks -ferritin 500–800 μg/l and/or TSAT 30–50%: 100 mg of iron/monthly -ferritin> 800 μg/l and/or TSAT>50%: no iron. Hb, TSAT, Ferritin and PCR evaluation every 4 weeks. Results after switching from iron gluconate to FCM, Hb levels were stable or improved, reaching a significantly higher percentage of target patients (from 60% to 80% with Hb > 10,5 g/l). The switch was also associated with a significant improvement of iron status, unrelated to iron dose: the percentage of patients with a target TSAT (TSAT >=20%) has doubled after six months, moving from 30% to 70%, while the average consumption trend of FCM decreasing over time (-48% after six months). It was also shown a marked reduction in ESA consumption: the ESA dose was decreased on average by -1907 IU per patient/month. Conclusion The switch from iron gluconate to FCM is associated with a better control of iron status and iron anemia in CKD patients on hemodialysis. The treatment schedule proposed has guaranteed to reach the primary and secondary endpoints, underlining the importance and the effectiveness of a tailored therapeutic protocol.

Sustained Local Diversity of Vibrio cholerae O1 Biotypes in a Previously Cholera-Free Country

ABSTRACT Although the current cholera pandemic can trace its origin to a specific time and place, many variants of Vibrio cholerae have caused this disease over the last 50 years. The relative clinical importance and geographical distribution of these variants have changed with time, but most remain in circulation. Some countries, such as Mexico and Haiti, had escaped the current pandemic, until large epidemics struck them in 1991 and 2010, respectively. Cholera has been endemic in these countries ever since. A recent retrospective study in mBio presents the results of more than 3 decades of V. cholerae monitoring from environmental and clinical sources in Mexico (S. Y. Choi et al., mBio 7:e02160-15, 2016, http://dx.doi.org/10.1128/mBio.02160-15 ). It reveals that multiple V. cholerae variants, including classical strains from the previous pandemic, as well as completely novel biotypes, have been circulating in Mexico. This discovery has important implications for the epidemiology and evolution of V. cholerae .

Desialylation: A Novel Platelet Clearance Mechanism and a Potential New Therapeutic Target in Anti-GPIb Antibody Mediated Thrombocytopenia

Abstract 265 Background: Immune thrombocytopenia (ITP) is an autoimmune disease characterized by autoantibodies directed at patient's own platelet antigens, primarily glycoprotein (GP)IIbIIIa-integrin (70–80%) and GPIb-complex (20–40%). Current paradigm suggests that clearance of opsonized platelets through the reticuloendothelial system via Fcγ-receptors results in thrombocytopenia and bleeding disorders. However, evidence from others and our group demonstrated that anti-GPIbα, but not anti-GPIIbIIIa, can induce thrombocytopenia via an Fc-independent pathway, which is resistant to intravenous IgG (IVIG) therapy in murine ITP-models (Blood 2006). These observations are consistent with subsequent IVIG studies in human ITP patients. Interestingly, human anti-GPIb-mediated ITP patients seem also resistant to steroid therapy in our recent retrospective study (American Journal of Hematology 2012). This suggests that binding of anti-GPIbα antibodies may induce platelet clearance through a different mechanism which is currently poorly understood. Methods: We developed unique mouse anti-mouse monoclonal antibodies (mAbs) in GPIIIa or GPIba deficient mice. Some of the mAbs have cross-reactivity to both mouse and human GPIIbIIIa and GPIba. Flow cytometry was used to evaluate whether these mAbs were able to induce platelet activation, apoptosis and desialylation. GPIbα is heavily glycosylated and the role of desialylation and exposure of underlying galactose and β-N-acetyl-D-glucosamine (βGN) residues on GPIbα in platelet clearance was assessed using the sialidase neuraminidase (NA) and it's inhibitor N-acetyl-2,3-dehydro-2-deoxy neuraminic acid (DANA). Desialyation effects on platelet activation and apoptosis was measured by flow cytometry. We also repeated these experiments with human platelets and plasma from human ITP-patients. We also investigated the effects of anti-GPIbα antibodies on platelet activation, apoptosis and clearance in vivo. Briefly, BALB/c mice were injected with anti-GPIbαor anti-GPIIIa mAbs and 24 hrs later, platelet desialylation, activation and apoptosis were measured by flow cytometry. The effect of desialylation on platelet clearance was assessed with DANA. The possible roles of Ashwell-Morell and MAC-1 receptors in GPIbα-mediated platelet clearance in the liver were examined using immunohistochemistry (anti-CD11b) or blocking of the Ashwell-Morell receptor with asialofetuin. Results and Discussion: We found that anti-GPIbα, but not anti-GPIIbIIIa mAbs, induced significant P-selectin expression and phosphatidylserine (PS)-exposure, and increased inner membrane mitochondrial depolarization (ΔYm). Interestingly, platelets were desialylated in the presence of anti-GPIbα but not anti-GPIIbIIIa mAbs. Moreover, we found that desialylation of GPIbα lies directly upstream of platelet activation and apoptosis, as prior treatment with DANA diminished PS-exposure, and P-selectin expression. Most importantly, incubations of human platelets with ITP-patient plasma showed similar effects. In vivo, we found significant increases in PS-exposure and ΔYm induced by anti-GPIbα, but not by anti-GPIIIa mAbs, independent of IgG subclass. Interestingly, prior injection with DANA rescued platelets numbers in anti-GPIbα, but not in anti-GPIIIa injected mice. A significant role for the Ashwell-Morell and MAC-1 receptors in the clearance of deglycosylated platelets was observed; blocking of the Ashwell-Morell receptors by asialofetuin, decreased platelet clearance in anti-GPIbα, but not anti-GPIIbIIIa antibody injected mice, there was also increased staining for MAC-1 on Kupffer cells, exclusively in the presence of an anti-GPIbα mAb tested. Thus, we demonstrate for the first time that anti-GPIbα antibodies induce GPIbα desialyation, leading to platelet activation and apoptosis. Therefore, we identified novel Fc-independent platelet clearance pathways, more specifically, via Ashwell-Morell and MAC-1 receptors on hepatocytes and liver macrophages. These findings may lead to novel therapeutic regimens including the potential use of sialidase inhibitors as a solution for anti-GPIb-mediated ITP patients previously refractory to both steroid and IVIG therapies. Disclosures: No relevant conflicts of interest to declare.

Prognosis of Thyroid Cancer Related to Pregnancy: A Systematic Review

Differentiated thyroid cancer (DTC) is the second most common cancer in pregnancy. Its management is a challenge for both doctors and patients, and the best timing for surgery is unclear. A systematic review evaluating the prognosis of DTC in pregnant patients was conducted. After reviewing 401 unique citations and 54 full texts, 4 studies that compared the prognosis of patients with DTC related to pregnancy (DTC diagnosed during pregnancy or within 12 months after childbirth) or not were included. In two studies the primary outcome was overall survival, in one study the primary outcomes were recurrent disease and death related to thyroid cancer, and in one study the primary outcome was recurrent or persistent disease. In the first two studies, there was no difference in overall survival in patients with pregnancy-related DTC, when compared with matched controls; in one study, there was no difference in death caused by DTC nor recurrence in DTC related to pregnancy. Nevertheless, in a recent retrospective study, a higher rate of recurrent or persistent DTC was observed in patients with DTC related to pregnancy. There are not many studies on which to base treatment decisions in pregnant patients with DTC.

An Unusual Case of Stroke and Fevers in a Traveler Returning from Arizona

Primary coccidioidal infection caused by inhalation of spores growing several inches below the surface of desert soil in the San Joaquim valley in southern Arizona and central California is well documented in the literature. Most infections resolve quickly with minimal symptoms, although some individuals develop a subacute process called “Valley Fever”, which is characterized by shortness of breath, chest pain, cough and fevers lasting from weeks to months. Skin manifestations, including erythema nodosum and erythema multiforme may also be present and generally resolve with resolution of the respiratory tract illness. A recent retrospective study found that 6003 adult and 332 pediatric patients were hospitalized with endemic mycosis in 2002, but the overall incidence has been estimated at about 150,000 infections per year. We report a unusual case of recurrent stroke temporally associated with a CNS Coccidiomycosis infection in a traveler to a region where the fungus is endemic.