Viral Hepatitis Clinical Trial
Official title:
Viral Hepatitis B and C Infection in Patients With Idiopathic Thrombocytopenic Purpura Treated With Triple Therapy
Aim of the work To estimate frequency of viral HB & C infection in ITP patients who received
triple therapy in comparison with another group treated with steroids only.
To explore risk factors and routes of transmission of viral HB & C infection in ITP patients
who received triple therapy and the another group treated with steroids .
- To assess preventive measures of viral HB& C infection in the hematology ward To
investigate the influence of viral HB & C infection on clinical picture, response to
treatment and side effects in ITP patients who received triple therapy or steroids.
Primary immune thrombocytopenia (ITP) is an autoimmune disorder characterized by isolated
thrombocytopenia in the absence of other causes.ITP is mediated by antiplatelet
autoantibodies. Antibody-coated platelets are phagocytosed by macrophages in the
reticuloendothelial system, leading to accelerated platelet clearance. Macrophages also act
as antigen-presenting cells interacting with CD8+ and CD4+ T cells that in turn stimulate
antibody-producing B cells.This pathogenic loop sustains autoantibody production. T
cell-mediated platelet lysis and megakaryocyte immunoinjury contribute to the diverse
pathobiology of ITP.
Single-agent treatments have not been successful at inducing prolonged remission.With
immunosuppressive monotherapy, ITP patients usually require prolonged treatment, leading to
unpleasant and sometimes serious side effects.
Recent studies combining dexamethasone and rituximab in short courses have reported
encouraging results.it is postulated that adding cyclosporine to this combination may induce
a more enduring remission by also targeting T cells and thereby briefly suppressing all 3
immune cell types implicated in sustaining the pathogenic loop.
Suppressing these cells simultaneously has a risk of predisposing to serious infections.it is
considered it appropriate to conduct a pilot study on a small number of patients with the aim
of investigating the safety and efficacy of the triple therapy.
Infectious complications, mainly caused by the use of corticosteroids and other
immunosuppressive agents, are a major cause of morbidity in patients with cITP. Moreover,
infections may trigger autoimmune diseases and, at least theoretically, may be a complication
of an already impaired immune system. It has been reported that children have an increased
incidence of infection before diagnosis of ITP.
Hepatitis B (HBV) and C (HCV) virus infections are bloodâborne viruses that pose major public
health threats worldwide. The World Health Organization (WHO) report released in April 2017
on the status of hepatitis worldwide documented that 1.75 million new cases of HCV infection
occurred in 2015, with about 71 million people already infected, the Eastern Mediterranean
region has the highest HCV prevalence rate in the world According to WHO, in 2017 Egypt had
the highest HCV prevalence rate in the world . According to the IHME in 2016, there were
4,002,706 men and 3,757,236 women with chronic HCV. HCV prevalence was estimated to be 11.9%
among the general population (populations at relatively low risk of exposure to HCV, such as
healthy children, blood donors, antenatal clinic attendees and pregnant women), 55.6% among
populations at high risk (PWID, hemodialysis, multitransfused individuals and hemophiliacs),
14.3% among populations at intermediate risk (household contacts of HCV-infected individuals,
prisoners, individuals with diabetes and healthcare workers), 56.0% among populations with
liver-related conditions (acute viral hepatitis, liver cirrhosis, chronic liver disease,
hepatocellular carcinoma and non-Hodgkin's lymphoma) and 35.0% among special clinical
populations (dermatological manifestations, rheumatologic disorders and non-liver-related
malignancies Thrombocytopenia can also complicate bleeding manifestations such as variceal
bleeding. It may impede the initiation and continuation of antiviral therapy, potentially
decreasing the probability of successful HCV reatment.Recent studies have evaluated the
underlying mechanism of thrombocytopenia in chronic HCV infection and assessed the usefulness
of several therapeutic options.
Besides hepatic complications, chronic HCV infection is also associated with several
extra-hepatic manifestations including thrombocytopenia. Thrombocytopenia in chronic Hcv
infection is a major problem, particularly in patients with advanced liver disease. The risk
of serious bleeding with severe thrombocytopenia can prevent invasive procedures including
biopsies for staging.
The pathophysiology of thrombocytopenia in patients with HCV infection is thought to be
multifactorial. Besides inducing an autoimmune reaction with production of antiplatelet
antibodies, the virus also causes direct bone marrow suppression with resulting
thrombocytopenia , chronic HCV infection induced liver fibrosis and cirrhosis leads to portal
hypertension with subsequent hypersplenism and sequestration of platelets, decreased the
production of thrombopoeitin, and endothelial dysfunction, all of which can contribute to
thrombocytopenia.Although uncommonly used in developed countries, interferon (IFN) and
ribavirin used as part of anti-HCV therapy can also contribute to low platelet
count.Hepatitis B virus (HBV) infection represents a significant global health problem, since
almost one third of the worlds population has serological signs of previous or present
infection, and that 240 million individuals are chronic hepatitis B surface antigen (HBsAg)
carriers. Worldwide, low rates of serological HBsAg positivity (0.2%-0.5%) and signs of
previous HBV contact [4%-6% HBsAg negative/anti-hepatitis B core antigen antibodies
(anti-HBc)positive subjects] are registered in north western and central Europe, north
America and Australia. On the contrary, the highest prevalences are reported in China,
Southeast Asia and tropical Africa (chronicinfection 8%-20%, and previous exposure
70%-95%,respectively).
It is presently well known that medications such as glucocorticoids and anticancer treatments
can interfere with the host immune system and blunt the control that it exerts over HBV
replication, with the potential to cause viral reactivation (HBVr) in both HBsAg positive
patients and individuals with serological signs of previous resolved HBV exposure. HBVr can
assume various manifestations, spanning from asymptomatic hepatitis to life threatening
fulminant liver failure. This risk is most common among patients undergoing treatment for
hematological tumors or those receiving hematopoietic stem cell transplantation (HSCT).
Nevertheless, also patients with solid tumors, immunological diseases and inflammatory bowel
diseases are exposed to the risk of HBVr.The existence of an effective vaccination and a
mature treatment schedule for HBV suggests that the potential for elimination of this virus
as a major public health problem in Egypt exists. In a challenging economic climate,
effective targeting of prevention and treatment strategies for both HBV and HCV is essential
to make best use of limited resources in Egypt, however. Recent modelling work on HCV
illustrates the potential power of intervention targeting in both reducing the risk of
infection spread, and improving treatment outcomes, in the Egyptian context.
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