Classification and Pathogenesis of  Pre-eclampsia

Classification of Pre-eclampsia:

1. Mild Pre-eclampsia:

Is defined as systolic blood pressure (SBP) of at least 140 mmHg and/or diastolic blood pressure (DBP) of at least 90 mmHg on at least two occasions at least 6 hours apart after the 20th week of gestation in women known to be normotensive before pregnancy and before 20 weeks of gestation plus proteinuria (≥ 300 mg/24 h.). If 24 h. urine collection is not available, then proteinuria is defined as a concentration of at least 30 mg/dL (at least 1+ on dipstick) in at least two random urine samples collected at least 6 hours apart. 

➧ Serum urate levels are often elevated in pre-eclampsia. Hyperuricemia is associated with perinatal complications, and although elevated levels have not predicted adverse maternal outcomes, urate is frequently measured in clinical practice. 

2. Severe Pre-eclampsia:

Is defined as sustained elevations in SBP to at least 160 mmHg and/or in DBP to at least 110 mmHg for at least 6 hours in association with abnormal proteinuria or if there is hypertension in association with severe proteinuria (≥5 g/24 h.). In addition, pre-eclampsia is considered severe in the presence of multiorgan involvement such as pulmonary edema, oliguria (< 500 mL/24 h.), thrombocytopenia (platelet count < 100000 / mm³), abnormal liver enzymes in association with persistent epigastric or right upper quadrant pain, or persistent severe central nervous system (CNS) symptoms (altered mental status, headaches, blurred vision or blindness). 

➧ A severe variant of pre-eclampsia also features hemolysis, elevated liver enzymes, and low platelets (HELLP syndrome). This condition occurs in about 1/1000 pregnancies. Predisposing factors are positive family history, hypertension, diabetes, preexisting renal disease, multiple pregnancies, and poor obstetric history. Pre-eclampsia with hepatic dysfunction, without hemolysis, may occur in severe pre-eclampsia.

Pathogenesis of Pre-eclampsia:

➧ The etiology of preeclampsia remains unknown; however, defective remodeling of spiral arteries during trophoblast invasion is a recognized predisposing factor for pre-eclampsia. Abnormal trophoblast differentiation and incomplete invasion by the placenta of uterine blood vessels leads to the formation of a placenta in which uterine spiral arteries fail to undergo the normal thinning out of muscular walls that permits enhanced perfusion of the placenta. Thus, perfusion of the intervillous space is impaired, leading to placental hypoxia. 

➧ Pre-eclampsia is characterized by placental hypoxia and/or ischemia, excessive oxidative stress, in association with endothelial dysfunction. The release of soluble factors from the ischemic placenta into maternal plasma plays a central role in the ensuing endothelial dysfunction, the most prominent feature of this disease. 

➧ Endothelial dysfunction in pre-eclampsia results from an antiangiogenic state mediated by high circulating levels of soluble Fms-like tyrosine kinase-1 (sFlt-1) and soluble endoglin in concert with low levels of proangiogenic factors like placental growth factor (PlGF), vascular endothelial growth factor (VEGF). The placenta makes sFlt1 in large amounts, but circulating mononuclear cells are an extra source of sFlt1 in pre-eclampsia. 

➧ High-circulating levels of sFlt-1 predate the onset and the severity of pre-eclampsia. Thus sFlt1 acts as a potent inhibitor of VEGF and PIGF by binding these molecules in the circulation and other target tissues, such as the kidneys. Thus excessive sFlt-1 plays a central role in the induction of the pre-eclampsia phenotype as sFLt-1 decreases VEGF binding to its receptor which reduces phosphorylation of endothelial nitric oxide synthase (eNOS) by VEGF leading to reduced eNOS. 

Other Pathophysiologic Mechanisms:

Include immunologic intolerance between fetoplacental and maternal tissues, placental and endothelial dysfunction, immune maladaptation to paternal antigens, exaggerated systemic inflammatory response, maladaptation to the cardiovascular or inflammatory changes of pregnancy, dietary deficiencies, and genetic abnormalities. 

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Definition, Differentiation, and Risk factors of Pre-eclampsia

Definition:

➧ Pre-eclampsia is a multi-systemic disease unique to human pregnancy.

➧ The term pre-eclampsia refers to the new onset of hypertension (≥140/90 mmHg) and proteinuria after 20 weeks of gestation in previously normotensive, non-proteinuric women i.e. there is an involvement of one or more organ systems. 

➧ There is a resolution of the disease by three months postpartum i.e. it is specifically a complication of pregnancy. 

➧ Delivery of the baby and removing the placenta is currently the only definitive way of curing the condition. 

➧ The disease is responsible for considerable morbidity and mortality, complicating 5-8% of pregnancies. 

➧ With its systemic vasoconstriction, intravascular volume and protein depletion, and simultaneous retention of extravascular sodium and water, pre-eclampsia is of particular concern to anesthesiologists. 

➧ In addition to individual organ dysfunction, abnormalities in coagulation and edema of the brain, larynx, and lungs may occur.

Atypical Pre-eclampsia:

➧ Atypical cases arise at less than 20 weeks of gestation and over 48 hours after delivery and have signs and symptoms of pre-eclampsia without typical hypertension or proteinuria. 

➧ The condition of pre-eclampsia should be considered, in the absence of proteinuria, when gestational hypertension is present in combination with persistent symptoms or when laboratory tests yield abnormal results.

➧ Pre-eclampsia should be considered in any pregnant woman with a severe headache or new-onset epigastric pain.

➧ Under extremely rare circumstances, pre-eclampsia may develop before 20 weeks of gestation in the setting of a hydatidiform mole, multiple pregnancies, fetal or placental abnormalities, antiphospholipid syndrome, or severe renal disease.

Differentiation of Pre-eclampsia:

➧ Pre-eclampsia is classified within the broad category of hypertensive diseases of pregnancy:

1- Pre-existing or chronic hypertension: is present before and often during pregnancy.

2- Gestational hypertension: is defined as hypertension arising after 20 weeks of gestation, without any other organ system involvement. 

3- Hypertension in pregnancy may be caused by a variety of different pathologies; these include renal disease, pheochromocytoma, drug usage such as cocaine and amphetamines, and cardiovascular diseases such as coarctation, subclavian stenosis, aortic dissection, and vasculitis. 

➧ Other forms of severe hepatic dysfunction in pregnancy need to be differentiated from pre-eclampsia: 

1- Acute fatty liver of pregnancy: is a rare condition of pregnancy, which is not associated with hypertension. 

2- Hemolytic Uremic Syndrome (HUS) ⁄ Thrombotic Thrombocytopenic Purpura (TTP): should be differentiated from HELLP syndrome, as treatment interventions differ significantly. HUS ⁄ TTP is a clinical diagnosis defined by the presence of a pentad of features; microangiopathic hemolytic anemia, thrombocytopenia, neurological symptoms and signs, renal function abnormalities, and fever.

Risk factors:

1- Nulliparity 

2- Multifetal gestations 

3- Previous history of pre-eclampsia 

4- Obesity 

5- Diabetes Mellitus 

6- Vascular and connective tissue disorders like systemic lupus erythematosus and antiphospholipid antibodies 

7- Age >35 years at first pregnancy 

8- Smoking 

9- African-American race 

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