6 research outputs found
Mechanisms of venous thromboembolism in oral contraception
Department of Biochemistry and
Clinical Biochemistry, Nicolae Testemitanu State University of Medicine and Pharmacy,
Chisinau, Republic of Moldova, The 8th International Medical Congress for Students and Young Doctors, September 24-26, 2020Introduction. Combined oral contraceptives (COC) are more and more used by fertile women,
as well as teenagers in different cases, like dysmenorrhea, endometriosis, ovarian polycystic
syndrome, dysfunctional uterine bleeding (DUB) and hormone-replacement therapy (HRT) for
primary ovarian insufficiency. Even if they act efficiently in pregnancy prevention and
hormonal regulation, they also significantly increase the risk of venous thromboembolism.
Recent researches have shown that the risk of venous thromboembolism depends a lot on the
ratio of estrogen/progestin in combined oral contraceptives and on thrombotic events of women
on COC.
Aim of the study. Description of the mechanisms that can induce venous thromboembolism
and the selection of women potentially predisposed to them. Highlighting the frequency of their
occurrence depending on the ratio estrogen/progestin in the composition of combined oral
contraceptive. Individual prescription for oral contraceptives, in order to reduce their risk for
health.
Materials and methods. The literature analysis has been conducted using 98 bibliographic
sources from PubMed search engine starting with January 2017 and from PMC since January
2015.
Results. In women with mutation of Factor V Leiden and prothrombin, as well as defects of
antithrombin III, protein C and S, that take hormonal contraceptives, the risk of venous
thromboembolism increases up to 3-9%, unlike women who do not take them. Also, women
who take oral contraceptives with estrogen and levonorgestrel, deriving from progestin, have
a high level of Factor VII, X and fibrinogen, produced by high hepatic synthesis stimulated by
the first hepatic degradation of estrogen, and high APC resistance and low level of
antithrombine and protein S. Thus, favorable conditions for venous thromboembolism occur.
Conclusions. In women who take oral contraceptives the risk of thrombosis is higher than in
women who do not take them. The mechanisms inducing venous thromboembolism depend a
lot on the specific ratio of estrogen/progestin and the presence of hereditary or acquired
thrombophilia in women on COC
Sindromul tromboemboliei arterei pulmonare
Background. Pulmonary embolism is a common complication of deep vein thrombosis (DVT) or the
penetration of amniotic fluid into the maternal circulation. Risk factors include varicose vein disease of
the lower limbs, use of combined oral contraceptives or hormone replacement therapy. Objective of the
study. Differentiated estimation of the pathogenetic mechanisms, manifestations and complications of
pulmonary embolism, as well as the argumentation of a pathogenetic treatment to combat the
complications with risk for the patients' lives. Material and Methods. Study of a clinical case with
pulmonary embolism syndrome and literature analysis since 2017 January from
PubMed. Results. Repeated pulmonary embolism occurs during the migration of microthrombi from
deep thrombosed veins or when amniotic fluid passes into the maternal circulation. Following reactive
vasoconstriction, HTP (pulmonary hypertension) is rapidly installed, which will induce asymmetric
hypertrophic cardiomyopathy disease with cardiorespiratory failure. Dyspnoea with dry cough, chest
pain, tachycardia, and restlessness will also occur. Massive pulmonary embolism are usually
fatal. Conclusion. In people with untreated deep vein thrombosis, the risk of pulmonary embolism
increases and quickly may appear cardiorespiratory complications or a fatal end.
Introducere: Tromboembolia arterei pulmonare este o complicație des întâlnită a tromboemboliei
venoase profunde sau pătrunderea lichidului amniotic în circulația maternă. Printre factorii de risc se
numără boala varicoasă a membrelor inferioare, consumul de contraceptive orale sau terapia de
reînlocuire hormonală. Scopul lucrării. Estimarea diferențiată a mecanismelor patogenetice, a
manifestărilor și complicațiilor tromboemboliei, precum și argumentarea unui tratament patogenetic
pentru combaterea complicațiilor cu risc pentru viața pacienților. Material și Metode. Studiul unui caz
clinic cu sindromul tromboembolic pulmonar, analiza surselor bibliografice referitoare la temă din
PubMed, începând cu ianuarie 2017. Rezultate. Tromboembolia repetată a arterelor pulmonare apare la
migrarea microtrombilor din venele profunde trombozate sau la trecerea lichidului amniotic în circulația
maternă. În urma vasoconstricției reactive rapid se instalează HTP (hipertensiune pulmonară), care va
induce cardiopatie hipertrofică asimetrică cu insuficiență cardiorespiratorie. Concomitent, vor apărea:
dispnee cu tuse seacă, durere toracică, tahicardie și o stare de neliniște. De obicei, embolii masivi sunt
adesea fatali. Concluzii. La persoanele cu tromboze venoase profunde netratate crește riscul de
tromboembolie pulmonară care induce rapid complicații cardiorespiratorii sau un final fatal
Pulmonary embolism syndrome
State University of Medicine and Pharmacy "Nicolae Testemiteanu" Chișinău, Republic of Moldova, Congresul consacrat aniversării a 75-a de la fondarea Universității de Stat de Medicină și Farmacie „Nicolae Testemițanu” din Republica Moldova, Ziua internațională a științei pentru pace și dezvoltareIntroduction:
Pulmonary embolism is defined as an obstruction of the pulmonary vasculature
and is a subset of VTE that represents the third most common cause of vascular
disease after acute myocardial infarction and stroke. It is a common complication of
deep vein thrombosis (DVT) or the penetration of amniotic fluid into the maternal
circulation.
The incidence of PE increases with age. Men typically have a higher overall
incidence of VTE compared with women , but women have a higher incidence after
age 75. At the age of 45 years, there is a lifetime risk of venous thromboembolism of
8.1% with some patient subsets having even higher life time risk, such as African
Americans -11.5%, those that are obese - 10.9%, those identified to be heterozygous
for factor V Leiden - 17.1%, or those who have sickle cell disease - 18.2%.
The confirmed PE patients can be categorized and triaged according to the
presence or absence of the shock or hypotension., therefore PE can be high,
intermediate or low risk.
Risk factors include varicose vein disease of the lower limbs, use of combined
oral contraceptives or hormone replacement therapy. It usually occurs through small
thrombi that are diffused into the pulmonary capillary bed.
Purpose:
Differentiated estimation of the pathogenetic mechanisms, manifestations and
complications of pulmonary embolism, as well as the argumentation of a pathogenetic
treatment to combat the complications with risk for the patients' lives.
Material and methods:
Relevant articles from PubMed with latest update since 2017 january and a clinical
case with pulmonary embolism syndrome and its complications.
Clinical presentation:
The clinical presentations of PE are heterogeneous and range from asymptomatic in
incidentally discovered small subsegmental embolus to massive saddle embolism to
cardiogenic shock and/or sudden death in the context of massive saddle embolism.
Typical symptoms and/or signs include pleuritic chest pain, dyspnoea, fever, cough,
hemoptysis, and syncope.
Physical examination may reveal tachycardia, tachypnea, fever, and hypoxia, as
well as reduced breath sounds or rales, jugular venous distention, and right ventricular
(RV) heave.
Diagnostic evaluation:
Those with high-clinical suspicion, for example, patients presenting pleuritic chest
discomfort and dyspnea who have a history of malignancy and recent immobility that
manifest hypoxia, tachycardia, and hypotension and are unstable require a distinct
evaluation than those with low-clinical suspicion in whom typical symptoms and/or risk
factors are not present.
Basic evaluations often performed in these patients include:
•ECG which often, but not always, reveals sinus tachycardia, supraventricular
arrhythmias and right axis deviation in 15-25% patients.
•Chest X-ray (CXR) which may include enlarged PA (Fleischner sign), regional oligemia
(Westermark sign), and Hampton hump (wedge-shaped distal infarct).
• Clinical prediction rules, such as Wells score, modified Wells score and Geneva
scores.
•D-dimer test – a sensitive marker of thrombosis, which is used in low and intermediate
clinical probability.
•CTA – used in high clinical probability with hypotension ore shock, it has high
sensitivity and specificity in detecting PE.
•VQ scan is used in situations where CT scan is contraindicated, like pregnancy, acute
renal failure, and/or contrast allergy.
•Cardiac biomarkers, such as, cardiac troponins and BNP.
Pathophysiology:
The apperance of VTE is characterized by Virchow triad, which includes issues affecting endothelial injury,
stasis of blood flow, and hypercoagulability. Endothelial injury can result from surgery, trauma, venous
catheters, and superficial vein thrombosis. Stasis can be caused by prolonged immobilization during travel,
surgery, obesity, and polycythemia vera, with most emboli developing in the lower extremity veins.
Hypercoagulability can be either genetic (e.g., factor V Leiden mutation, prothrombin gene mutation,
antithrombin III deficiency, protein C, S deficiency, and increased homocysteine levels) or an acquired disorder
(e.g., antiphospholipid syndrome, infection, inflammatory conditions, cancer, nephrotic syndrome, smoking,
using of hormonal contraceptives, hormone replacement therapy, or pregnancy).
The thrombus lodges in the pulmonary arteries from a DVT and causes immediate mechanical obstruction.
The embolism activates the coagulation system, damages the endothelium, stagnate pulmonary blood flow and
accordingly initiate secondary pulmonary thrombosis which worsens the mechanical obstruction.
Mechanical obstruction of the pulmonary vasculature coupled with a complex interaction between humoral
factors from the activated platelets, endothelial effects, reflexes and hypoxia cause pulmonary vasoconstriction
that worsens RV afterload. Vasoconstrictors include serotonin, thromboxane, prostaglandins and endothelins,
counterbalanced by vasodilators such as nitric oxide and prostacyclins.
Hematogenous thromboembolism increases pulmonary arterial pressure (PAP) more effectively than nonhematogenous
material, emphasizing the importance of PE-released vasoconstrictors. Activated platelets and the
thrombus mass secrete thromboxane-A2, prostaglandins, adenosine, thrombin, and serotonin which induce
platelet aggregation and pulmonary vasoconstriction. Pulmonary endothelial cells inactivate serotonin and
certain prostaglandins to maintain homeostasis. Endothelins (ET) are produced by the pulmonary vascular
endothelium when it is stimulated by thrombin, endothelial injury and hypoxia. ET target the ETA and ETB
receptors in the smooth muscle cells, and pulmonary vasoconstriction is induced by activation of phospholipase
C that increases IP3, DAG and intracellular Ca+. ET have been estimated to be in charge of 25% of the PEinduced
increase in PVR, but findings are variable. ET also induce bronchoconstriction and release of TxA2
which further potentate the pulmonary vasoconstrictor effect.
Vasoconstriction from PE leads to ventilation–perfusion (VQ) mismatch and resulting hypoxia, which leads
to the elevation of PVR and pulmonary artery (PA) pressure. Elevated PA pressure results in the reduction in RV
stroke volume and RV dilatation. Elevated RV end-diastolic pressures cause neurohumoral stimulation,
increased oxygen demand, and resultant subendocardial hypoperfusion, myocardial ischemia, and subsequent
infarction. RV dilatation can lead to RV failure. Progression of RV failure can lead to impairment in left
ventricular filling and may result in myocardial ischemia due to inadequate coronary artery filling with the
appearance of hypotension, syncope, or sudden death. Hypoxia, elevated alveolar-arterial (A-a) gradient, and
hypocapnea are frequently observed in PE.
VQ mismatch, right to left shunt, impaired diffusion, and reduced mixed venous oxygen saturation all
togather contribute to hypoxia.
Importantly, not all patients are hypoxemic (32% of PE cases demonstrate PaO2 > 80 mmHg), and that the
majority of patients (81%) hyperventilate despite the increased dead space with nearly one-third of patients have
normal A-a gradient.
Management:
The use of D-dimer testing (a sensitive marker of thrombosis), computed tomographic pulmonary angiography,
echocardiography and cardiac biomarkers have facilitated the triage and management of patients with confirmed PE.
The initial treatment should begin with oxygenation and stabilization of the patient. Hereafter the management of PE
will continue using direct oral anticoagulants (DOACs) , thrombolytic therapy and catheter-based therapies, with or
without fibrinolysis, that have emerged as potential options to treat higher-risk, unstable patients.
Exogenous administration of pulmonary vasodilators in acute pulmonary embolism seems attractive but all come with
a risk of systemic vasodilation or worsening of pulmonary ventilation-perfusion mismatch.
Clinical case:
A 58 years female with pulmonary cardiomiopathy induced by multiple
thromboembolism of pulmonary vessels (massive embolism of left lung), respiratory failure
(II-III level) with high risk of assimetric hypertrophic cardiomiopathy and minimal
obstruction of left ventricular ejection tract. AHT level III. Mitral failure level II. Cardiac
failure level III (NYHA). Right atrium is considerably dilated, but righr ventriculum is
weakly modified. Pericardial liquid and high PHT.
Furthermore she has varicose disease of lower limbs (level II) with deep vein
thrombosis, which have induced the appearance of pulmonary embolism; also depressiveanxiety
syndrome and chronic iron deficiency anemia.
Symptoms: dyspnoea in minimal effort, cough, fever, muco-purulent sputum and
hemoptysis, palpitations, general asthenia, high blood pressure, cyanotic teguments,
periumbilical cyanosis, face and lower limbs edema, low vesicular murmur and bilateral
basal crackling rales.
Special investigations: D-dimer test – negativ, alchalin phosphatase – 143 U/L, dimol
test – 1,2 nn.
EKG: sinusal rhythm, sinusal tachycardia, pulmonare P in DII, DIII and AVF, and right
atrium hypertrophy. ;
8 years ago has appeared the first access of asphyxia, dyspnoea and severe chest pain.
Since then she annually is hospitalized.
During whole hospitalization the signs haven’t improved., but the cardiorespiratory
failure has worsen even more, therefore she was connected to oxygen mask. Blood pressure
varies between 130-100 mmHg (systolic) si 90-70 mmHg (diastolic).
Treatment: Ca+ antagonists, anticoagulants, antiagregants, diuretics, Ca+ and Fe+
medicaments and O2 therapy.
After hospitalization all the symptoms have been improved for a time.
Results:
The clinical case and a lot of relevant scientific articles highlights that in people with
untreated deep vein thrombosis, the risk of pulmonary embolism increases significantly and
quickly may appear cardiorespiratory complications or a fatal end. Also massive PE can
markedly increase physiological dead space and impair CO2 exchange.
Conclusion:
PE is a relatively common disorder causing significant morbidity and mortality, induced
by right ventricular (RV) failure, which is caused by a combination of mechanical obstruction
and pulmonary vasoconstriction, which both increases RV afterload. By combining patient
presentation, clinical suspicion, and various scoring systems, diagnosis may be streamlined
and a focused treatment can be instituted. Increasingly more physicians possess training and
have access to portable ultrasound devices, which may help in the early recognition and
treatment of VTE and PE. The increased accuracy of CTA and application of guidelinedirected
therapies have improved the recognition of PE in patients. Several newer oral
anticoagulation drugs are now available and gaining favor among physicians either because
they are safer or because they are easier to administrate without periodic monitorization of
anticoagulation status
Autoimmune associations of non-Hodgkin lymphomas
Universitatea de Stat de Medicină şi Farmacie „Nicolae Testemiţanu”, Chişinău, Republica MoldovaIntroducere. Bolile autoimune și hemopatiile maligne au în comun multiple tangențe etiopatogenetice, clinice și legate de tratament. În fiecare boală autoimună există o stimulare antigenică cronică, mai devreme sau mai târziu aceasta ar putea fi ca trigger pentru activarea mecanismului de policlonare a limfocitelor B. Scopul lucrării. Studierea componentului autoimun în limfoamele non-Hodgkin (LNH) pentru relevarea particularităților clinice, paraclinice și evolutive ale lor. Material și metode. Au fost examinate 64 cartele de ambulatoriu ale pacienților cu diagnosticul confirmat morfologic și imunohistochimic de LNH, luați la evidență în IO (2020-2022). În acest context tipul LNH fiind stabilit în baza examenului morfologic și imunohistochimic, iar prezența componentului autoimun în baza consulturilor și investigațiilor specifice. Rezultate. Componentul autoimun a fost apreciat mai frecvent la pacienții cu LNH indolente-58%, stadiile IV-88,3%, cu simptoame B prezente-71,4%, de peste 60 de ani, femei-69%, din mediul urban-58%. În 82,7% cazuri a fost apreciat un singur component autoimun cu predominarea anemiei hemolitice autoimune (AHA) în 53,1%, fiind urmată de trombocitopenia autoimună (TA)16,7% și tiroidita autoimună-12,9%. De remarcat e faptul că în peste 50% componentul autoimun s-a dezvoltat concomitent cu diagnosticul LNH. Concluzii. Au fost apreciate 8 tipuri de componente autoimune, dezvoltate concomitent sau înainte de dezvoltarea LNH. AHA și TA s-au asociat cel mai frecvent. Acestea prevalează independent de vârstă, gender și preponderent la populația rurală.Background. Autoimmune diseases and hematological malignancies share multiple etiopathogenetic, clinical and treatment-related tangents. In every autoimmune disease there is a chronic antigenic stimulation, eventually this could be a trigger for the activation of the polyclonal mechanism of B-lymphocytes. Objective of the study. Study of the autoimmune component in non-Hodgkin’s lymphomas (NHL) to reveal their clinical, paraclinical and evolutionary features. Material and methods. Sixty-four outpatient charts of patients with morphologically and immunohistochemically confirmed diagnosis of NHL, recorded in IO (2020-2022), were examined. In this context, the type of NHL is established based on the morphological and immunohistochemical examination, and the presence of the autoimmune component based on specific consultations and investigations. Results. The autoimmune component was appreciated more frequently in patients with indolent NHL- 58%, stages IV - 88.3%, with present B symptoms 71.4%, over 60 years old, women - 69%, from the urban environment - 58 %. In 82.7% of cases, a single autoimmune component was appreciated with the predominance of autoimmune hemolytic anemia (AHA) in 53.1%, followed by autoimmune thrombocytopenia (AT) - 16.7% and autoimmune thyroiditis - 12.9%. It should be noted that in over 50% the autoimmune component developed simultaneously with the diagnosis of NHL. Conclusion. Eight types of autoimmune components developed concurrently or before the development of NHL, were evaluated. AHA and TA were most frequently associated. They prevail independently of age, gender and predominantly in the urban population
The prevalence of drug use among students of Iasi (English version)
The purpose of the research is to estimate the number of drug users among students of the universities from Iasi, to identify students' behavior towards the use of drugs, drug purchase offer, solutions to reduce the use of drugs. Research using mix methods for estimating the number of drug users using a representative survey, the use of focus groups to obtain qualitative information.Drugs, mix methods, survey, prevalence, students, weed shops