RESUMEN
Abstract Focal Adhesion Kinase (FAK) protein participates in proliferation, migration, cell survival, and apoptosis process. It has been described as overexpressed in several neoplasms being a promising target for therapy. BCR-ABL negative chronic Myeloproliferative Neoplasms (MPN) are clonal disorders characterized by the excess of proliferation and apoptosis resistance. The identification of the acquired JAK2 V617F mutation in MPN patients allowed a better understanding of pathogenesis. However, there is still no pharmacological treatment that leads all patients to molecular remission, justifying new studies. The present study aimed to evaluate FAK involvement in the viability and apoptosis of HEL and SET-2 cells, both JAK2 V617F positive cell lines. The FAK inhibitor PF 562,271 was used. Cell viability was determined using MTT assay and apoptosis verified by cleaved PARP, cleaved Caspase 3 and Annexin-V/PI staining detection. FAK inhibition significantly reduced HEL and SET-2 cells viability and induced apoptosis. Considering the role of JAK/STAT pathway in MPN, further investigation of FAK participation in the MPN cells proliferation and apoptosis resistance, as well as possible crosstalk between JAK and FAK and downstream pathways may contribute to the knowledge of MPN pathophysiology, the discovery of new molecular targets, and JAK inhibitors resistance mechanisms.
Asunto(s)
Apoptosis , Proteína-Tirosina Quinasas de Adhesión Focal/análisis , Janus Quinasa 2/efectos adversos , Pacientes/clasificación , Línea Celular/clasificación , Neoplasias/patologíaRESUMEN
As neoplasias mieloproliferativas crônicas (NMPC) são doenças hematopoiéticas clonais que acometem a linhagem mieloide. De acordo com a Organização Mundial de Saúde (OMS), a policitemia vera (PV), a trombocitemia essencial (TE) e a mielofibrose (MF) são classificadas como NMPC BCR-ABL negativas. O surgimento dessas doenças está correlacionado com fatores genéticos, como mutações nos genes JAK2, MPL e CALR e outras mutações cooperantes que também podem estar presentes, levando ao aparecimento de diferentes fenótipos e prognósticos. A OMS constantemente revisa e atualiza os critérios de classificação, levando em consideração aspectos clínicos, morfológicos e genéticos. As análises laboratoriais, hematológicas e genéticas são de grande importância para o diagnóstico das neoplasias hematológicas, e devem ser realizadas da forma correta para permitir o diagnóstico diferencial entre outras neoplasias e distúrbios reacionais. O presente trabalho tem como objetivo revisar a fisiopatologia das NMPC e relacionar com os achados clínicos, hematológicos e genéticos, visando instruir e atualizar os analistas clínicos para que possam efetivamente contribuir para o diagnóstico dessas doenças, impactando o prognóstico dos pacientes. Ainda, a discussão sobre diagnóstico molecular tem o intuito de chamar a atenção para a constante evolução da área e importância desta para a hematologia.
The Chronic Myeloproliferative Neoplasms (MPN) are hematopoietic disease that affect the myeloid lineage cells. According to WHO, the Polycythemia vera (PV), Essential Thrombocythemia (ET) and Myelofibrosis (MF) are classified as BCR-ABL negative neoplasms. The occurrence of these diseases is correlated with genetics factors, as mutations in the JAK2, MPL e CALR genes and other cooperative mutations that may also be present, leading to different phenotypes manifestations and prognostics. WHO revises and updates constantly these diseases' classification criteria, considering clinical, morphological and genetic aspects. Laboratory tests, both hematological and genetic, have a key rule at these diseases' diagnosis and must be performed correctly in order to ensure a differential diagnosis from other neoplasms and reactive disorders. This manuscript aims to revise the MPN's physiopathology linking it to clinical, hematological and genetical findings, aiming to instruct and update clinical analysts so they can contribute to those diseases' diagnostic, impacting the patients' prognostics. Furthermore, the considerations about molecular diagnostics have the intention of emphasize the constant evolution of this subject and its importance to hematology.
RESUMEN
Abstract This work presents the results of a device, MilkTech, developed to detect milk tampering, based on electrical measurements. The device indicates possible frauds by water, sodium chloride, caustic soda, ethyl alcohol and sodium bicarbonate. The advantages in relation to traditional methods are portability, low cost and detection of mixed frauds. The experiments were conducted in dairy plants at Governador Valadares, in Brazil. The results were compared with cryoscopy and chloride tests. It is demonstrated there is high correlation between MilkTech and Cryoscopy. For instance, the detection limit of the equipment for water addition with the set of analyzed data was 0.78% with precision of 1.1%. Adulterations with sodium chloride, caustic soda, ethyl alcohol and sodium bicarbonate are detected qualitatively, even when added with water, and MilkTech indicates "SUSPECT" milk.