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The cause of preeclampsia is unknown.
The maternal disease is characterized by
• Vasospasm
• Activation of the coagulation system
• Perturbations in humoral and autacoid systems
related to volume and blood pressure control
• Oxidative stress and inflammatory-like responses
• Pathologic changes that are ischemic in nature
Pathophysiology
Of importance, and distinguishing
preeclampsia from chronic or gestational
hypertension, is that preeclampsia is
more than hypertension; it is a systemic
syndrome, and several of its
“nonhypertensive” complications can be
life-threatening when blood pressure
elevations are quite mild.
Pathophysiology (cont.)
Heart: Generally unaffected; cardiac decompensation
in the presence of preexisting heart disease.
Kidney: Renal lesions (glomerular endotheliosis);
GFR and renal blood flow decrease; hyperuricemia;
proteinuria may appear late in clinical course;
hypocalciuria; alterations in calcium regulatory
hormones; impaired sodium excretion; suppression
of renin angiotensin system.
Pathophysiology (cont.)
Coagulation System: Thrombocytopenia; low
antithrombin III; higher fibronectin.
Liver: HELLP syndrome (hemolysis, elevated ALT
and AST, and low platelet count).
CNS: Eclampsia is the convulsive phase of
preeclampsia. Symptoms may include headache
and visual disturbances, including blurred vision,
scotomata, and, rarely, cortical blindness.
Pathophysiology (cont.)
• Documentation of HBP before conception or
before gestational week 20 favors a diagnosis of
chronic hypertension (essential or secondary).
• HBP presenting at midpregnancy (weeks 20 to
28) may be due to early preeclampsia, transient
hypertension, or unrecognized chronic
hypertension.
Differential Diagnosis
High-risk patients presenting with normal BP:
• Hematocrit
• Hemoglobin
• Serum uric acid
• If 1+ protein by routine urinalysis (clean catch)
present obtain a timed collection for protein and
creatinine
• Accurate dating and assessment of fetal growth
• Baseline sonogram at 25 to 28 weeks
Laboratory Tests
• Platelet count
• Serum creatinine
Patients presenting with hypertension before
gestation week 20:
• Same tests as described for high-risk
patients presenting with normal BP
• Early baseline sonography for dating and
fetal size
Laboratory Tests (cont.)
Laboratory Tests (cont.)
Patients presenting with hypertension after
midpregnancy:
• Quantification of protein excretion
• Hemoglobin and hematocrit and platelet count
• Serum creatinine, uric acid, and transaminase level
• Serum albumin, LDH, blood smear, and coagulation
profile

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Causes and characteristics of preeclampsia

  • 1. The cause of preeclampsia is unknown. The maternal disease is characterized by • Vasospasm • Activation of the coagulation system • Perturbations in humoral and autacoid systems related to volume and blood pressure control • Oxidative stress and inflammatory-like responses • Pathologic changes that are ischemic in nature Pathophysiology
  • 2. Of importance, and distinguishing preeclampsia from chronic or gestational hypertension, is that preeclampsia is more than hypertension; it is a systemic syndrome, and several of its “nonhypertensive” complications can be life-threatening when blood pressure elevations are quite mild. Pathophysiology (cont.)
  • 3. Heart: Generally unaffected; cardiac decompensation in the presence of preexisting heart disease. Kidney: Renal lesions (glomerular endotheliosis); GFR and renal blood flow decrease; hyperuricemia; proteinuria may appear late in clinical course; hypocalciuria; alterations in calcium regulatory hormones; impaired sodium excretion; suppression of renin angiotensin system. Pathophysiology (cont.)
  • 4. Coagulation System: Thrombocytopenia; low antithrombin III; higher fibronectin. Liver: HELLP syndrome (hemolysis, elevated ALT and AST, and low platelet count). CNS: Eclampsia is the convulsive phase of preeclampsia. Symptoms may include headache and visual disturbances, including blurred vision, scotomata, and, rarely, cortical blindness. Pathophysiology (cont.)
  • 5. • Documentation of HBP before conception or before gestational week 20 favors a diagnosis of chronic hypertension (essential or secondary). • HBP presenting at midpregnancy (weeks 20 to 28) may be due to early preeclampsia, transient hypertension, or unrecognized chronic hypertension. Differential Diagnosis
  • 6. High-risk patients presenting with normal BP: • Hematocrit • Hemoglobin • Serum uric acid • If 1+ protein by routine urinalysis (clean catch) present obtain a timed collection for protein and creatinine • Accurate dating and assessment of fetal growth • Baseline sonogram at 25 to 28 weeks Laboratory Tests • Platelet count • Serum creatinine
  • 7. Patients presenting with hypertension before gestation week 20: • Same tests as described for high-risk patients presenting with normal BP • Early baseline sonography for dating and fetal size Laboratory Tests (cont.)
  • 8. Laboratory Tests (cont.) Patients presenting with hypertension after midpregnancy: • Quantification of protein excretion • Hemoglobin and hematocrit and platelet count • Serum creatinine, uric acid, and transaminase level • Serum albumin, LDH, blood smear, and coagulation profile