1. OBSTETRICIANS AND CEREBRAL PALSY BY
DR.MAMTA RATH DATTA
Tata Main Hospital,
Jamshedpur.
2. DEFINITION A group of chronic disorders impairing control of
movement that appear in the first few years of life and
generally do not worsen over time.
3. Epidemiology� Incidence : 2 per 1000 live births.
90% cases : No intrapartum cause found.
Remaining 10% cases: Hypoxia may have had antenatal/intrapartum origins.
4. ETIOLOGY Congenital : 85%
Acquired : 15%
Genetic : small % age
5. PRENATAL FACTORS Maternal pathology :
Systemic diseases.
Prenatal nutrition.
Infections (TORCH).
Trauma.
CO poisoning.
6. Contd. FETAL CONDITIONS
- twinning
- arterial occlusion in utero
- blood dyscrasias
7. Contd. PLACENTAL & CORD ABNORMALITIEs
chronic placental insufficiency
true knots/tight cord around neck
abruptio placentae.
chorioamnoinitis.
8. Perinatal factors Prematurity/LBW
ICH/skull #
Breech
Neryous system malformations.
9. POSTNATAL FACTORS CNS infections
Head injury
ICH/Thrombosis
Late onset/mistreated hydrocephalous
Toxic poisoning
10. TYPES OF LESIONS
Pre/Sub/Ependymal .
Encepholopathy.
Neuropathy.
11. CLASSIFICATION BY GEOGRAPHIC INVOLVEMENT
Quadriplegia: basal nuclei,brain stem,cortical lesions.
Hemiplegia:periventricular
Diplegia: periventricular (commonest)
12. CLASSIFICATION(Contd.) By physiologic type:
SPASTIC: Cortex
ATHETIOD: Basal ganglion
ATAXIC: Cerebellum
HYPOTONIC: Cerebellum
MIXED
13. Problems in defining the cause & timing of neuropathology of CP. CP not diagnosed until mths./yrs. after birth.
Retrospective review.
Signs of fetal compromise neither sensitive nor specific to a cause/timing of the cause.
Proven metabolic acidemia can be due to a chronic/acute hypoxic event.
14. CRITERIA TO DEFINE ACUTE INTRAPARTUM HYPOXIC EVENT Essential criteria :
Intrapartum umbilical arterial cord blood pH < 7 and base deficit = > 12 mmol/ l.
Early onset severe or mod. neonatal encephalopathy in infants >34 wks.
Spastic quadriplegic or dyskinetic CP
15. Contd.
Non specific additional criteria:
Sentinel hypoxic event occuring just before or during labour.
Sudden deterioration of FHR following the above event
AS – 0-6 > 5 mins.
Early evidence of multisystem involvement
Early imaging evidence of acute cerebral abnormality
16. Predicting CP in Neonatal Nursery Term babies: Clinical staging by Sarnat(’76) .
Preterm babies:(Lacey et al,’97)
Coarse jitters.
Asymmetrical neck reflex.
Stereotypical repetive movements.
Hypertonia.
17. DIAGNOSIS Test motor skills
Check infants’ medical history
Reflexes
Hand preference
Rule out other disorders causing movement problems
18. INVESTIGATIONS CT Scan
MRI / Magnetic resonance spectroscopy
Ultrasound
19. PATHOPHYSIOLOGY Dec. C.B.F. – hypoxia / ischemia of brain
Opening of calcium channels
Inc. in lactate due to anaerobic glycolysis
Dec high energy phosphates
20. Contd.
Redistibution of CO,inc. CBF at the cost of autoregulation leads to cerebral edema
Inc. glutamate conc. causes rapid and delayed cell death by osmotic lysis & free radical activation
21. Management Preventive mgt.
Neuroprotection:
Mag.Sulf.
Steroids.
Excitatory amino acid inhibitors.
Conventional therapy for CP.
22. Malpractice Claims
Is cerebral palsy preventable?
23. MALPRACTICE CLAIMS Find out , if possible, the reasons behind the decision for claim
Offer to meet parents and to go thru’ clinical history
Evaluate the child’s current condition
Study neonatal records
Review obst. care
24. Conclusion
Large majority of pathologies are multifactorial & mostly unpreventable reasons during fetal development and neonatal period.
