convulsivedisorder in pediatrics pdf and ppt
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About This Presentation
neonatal convulsions
Slide Content
CONVULSIVE
DISORDER
DISORDER
INTRODUCTION
◦The word convulsion (or seizures) describes an involuntary
violent spasms, or a series of jerking of face, trunk, or
extremities with or without loss of consciousness, sensory,
autonomic or behavioral disturbances.
◦The word epilepsy describes a syndrome of recurrent
unprovoked, seizure unrelated to fever or to acute “cerebral
insult”.
◦The word convulsion (or seizures) describes an involuntary
violent spasms, or a series of jerking of face, trunk, or
extremities with or without loss of consciousness, sensory,
autonomic or behavioral disturbances.
◦The word epilepsy describes a syndrome of recurrent
unprovoked, seizure unrelated to fever or to acute “cerebral
insult”.
◦Status epilepticus (SE) iaa severe form of seizure
activity lasting more than 30 minutes or recurrent
seizures with failure to recover consciousnessbetween
repeated attacks.
activity lasting more than 30 minutes or recurrent
seizures with failure to recover consciousnessbetween
repeated attacks.
DEFINATION
◦Neonatal seizure is defined clinically as “ a paroxysmal
alteration in neurological function (i.ebehavioral, motor or
autonomic function)either or all three, occurring within 28
days.
◦In general: a convulsive or seizure is a paroxysmal
manifestations of neurological dysfunction.
◦Neonatal seizure is defined clinically as “ a paroxysmal
alteration in neurological function (i.ebehavioral, motor or
autonomic function)either or all three, occurring within 28
days.
◦In general: a convulsive or seizure is a paroxysmal
manifestations of neurological dysfunction.
INCIDENCE
Full term baby-3 in 1000
Pre-term baby-60 in 1000
Infants with birth weight <1500g :57.5/1000
Infants with birth weight between 2500g to 3999g : 2.8/1000
12000 are under the age of 18 years
Incidence is higher under 2 years and over age of 65years.
Full term baby-3 in 1000
Pre-term baby-60 in 1000
Infants with birth weight <1500g :57.5/1000
Infants with birth weight between 2500g to 3999g : 2.8/1000
12000 are under the age of 18 years
Incidence is higher under 2 years and over age of 65years.
RISK FACTORS
MAJOR
Age < 1 year
Prolonged fever
Hyper pyrexia
Infections
MINOR
Family h/o of febrile seizures
Family h/o of epilepsy
Complex febrile seizures
Male gender
Electrolytes imbalance
MAJOR
Age < 1 year
Prolonged fever
Hyper pyrexia
Infections
MINOR
Family h/o of febrile seizures
Family h/o of epilepsy
Complex febrile seizures
Male gender
Electrolytes imbalance
ETIOLOGY
NON RECURRENT (ACUTE)
•Febrile episode
•Intracranial infections
•Intracranial hemorrhage
•Cerebral edema
•Brain tumors
•Anoxia
•Toxins e.g.. Drugs, tetanus, lead
•Metabolic alterations
•Hyperbilirubinemia
RECURRENT (CHRONIC)
◦Idiopathic
◦Trauma
◦Infections
◦Congenital defects
◦Parasite brain diseases
◦Hormonal disorders
◦Hepatic disorder
◦Allergy
◦Sensory stimulus
◦Migraine
NON RECURRENT (ACUTE)
•Febrile episode
•Intracranial infections
•Intracranial hemorrhage
•Cerebral edema
•Brain tumors
•Anoxia
•Toxins e.g.. Drugs, tetanus, lead
•Metabolic alterations
•Hyperbilirubinemia
RECURRENT (CHRONIC)
◦Idiopathic
◦Trauma
◦Infections
◦Congenital defects
◦Parasite brain diseases
◦Hormonal disorders
◦Hepatic disorder
◦Allergy
◦Sensory stimulus
◦Migraine
PATHOPYSIOLOGY
RISK FACTORS AND ETIOLOGICAL FACTORS
ALTERED INTEGRITY OF NEURON IN THE EPILEPTOGENIC FOCUS
HYPEREXCITABILITY OF NEURONS
PARTIAL DEPOLORIZATION
RISK FACTORS AND ETIOLOGICAL FACTORS
ALTERED INTEGRITY OF NEURON IN THE EPILEPTOGENIC FOCUS
HYPEREXCITABILITY OF NEURONS
PARTIAL DEPOLORIZATION
PARTIAL STIMULATIONS OF NEUROTRANSMITTER MOLECULES
IMBALANCED RELEASE OF EXCITATORY AND INHIBITORY
NEUROTRANSMITTERS
LOWERED SEIZURES THRESHOLD
ABNORMAL SPONTANEOUS SPREAD OF ELECTRICAL DISCHARGE
CLINICAL MANIFESTATIONS
IMBALANCED RELEASE OF EXCITATORY AND INHIBITORY
NEUROTRANSMITTERS
LOWERED SEIZURES THRESHOLD
ABNORMAL SPONTANEOUS SPREAD OF ELECTRICAL DISCHARGE
CLINICAL MANIFESTATIONS
CONVULSION CLASSIFICATIONS AND
CLINICAL MANIFESTATIONS
FEBRILE CONVULSIONS
◦It refers to the seizures associated with feverbut excluding those
related to CNS infections. Common cause of convulsions in early
childhood (6 months to 5 years of age).
◦It has two types
◦Typical and Atypical
CLINICAL MANIFESTATIONS
FEBRILE CONVULSIONS
◦It refers to the seizures associated with feverbut excluding those
related to CNS infections. Common cause of convulsions in early
childhood (6 months to 5 years of age).
◦It has two types
◦Typical and Atypical
Typical or simple febrile
convulsions
Brief < 15 minutes
Occurs as a solitary event (one
attack/ 24 hours)
Typically generalized tonic-
clonicconvulsuions
Followed by a brief period of
postictal drowsiness
EEG are normal after the attack
Atypical febrile or
complex convulsions
Long > 15 minutes
Repeated convulsions for
several hours a day
May be focal or generalized,
tonic-clonicconvulsions
Followed by a long period of
postictal drowsiness
EEG show abnormal for 2
weeks after the attack
convulsions
Brief < 15 minutes
Occurs as a solitary event (one
attack/ 24 hours)
Typically generalized tonic-
clonicconvulsuions
Followed by a brief period of
postictal drowsiness
EEG are normal after the attack
Atypical febrile or
complex convulsions
Long > 15 minutes
Repeated convulsions for
several hours a day
May be focal or generalized,
tonic-clonicconvulsions
Followed by a long period of
postictal drowsiness
EEG show abnormal for 2
weeks after the attack
SEIZURE CLASSIFICATIONS AND
CLINICAL MANIFESTATIONS
Generalized seizures
1.Tonic-clonicalseizures
(grand mal)
2.Absence seizures
3.Atopic seizures
4.Myoclonic seizures
Partial seizures
1.Simple partial seizures
With elementary symptoms
No impaired consciousness
With motors signs (jacksonians)
With somatory-sensory-visual or
auditory
With autonomic manifestations
(abdominal) epilepsy
2. complex partial seizures
Includes psychomotor or temporal lobe
seizures
With impaired consciousness
CLINICAL MANIFESTATIONS
Generalized seizures
1.Tonic-clonicalseizures
(grand mal)
2.Absence seizures
3.Atopic seizures
4.Myoclonic seizures
Partial seizures
1.Simple partial seizures
With elementary symptoms
No impaired consciousness
With motors signs (jacksonians)
With somatory-sensory-visual or
auditory
With autonomic manifestations
(abdominal) epilepsy
2. complex partial seizures
Includes psychomotor or temporal lobe
seizures
With impaired consciousness
DIAGNOSTIC EVALUATIONS
HISTORY TAKING
Maternal history
Family history
Labourand delivery history
Baby conditions at birth
NEONATAL EXAMINATION
General examination
Neurological examination
CBG
Spo2
METABOLIC WORK UP
INFECTIONS WORK UP
CBC
CULTURE
Torch
Igm
CRP
BLOOD GAS ANALYISIS
INBORN ERRORS OF METABOLISM
CT-SCAN
MRI
EEG
LUMBAR PUNCTURE
HISTORY TAKING
Maternal history
Family history
Labourand delivery history
Baby conditions at birth
NEONATAL EXAMINATION
General examination
Neurological examination
CBG
Spo2
METABOLIC WORK UP
INFECTIONS WORK UP
CBC
CULTURE
Torch
Igm
CRP
BLOOD GAS ANALYISIS
INBORN ERRORS OF METABOLISM
CT-SCAN
MRI
EEG
LUMBAR PUNCTURE
COMPLICATIONS
Cranial nerve palsies
Raised ICP
Subdural effusion
Cerebral palsy
Hydrocephalus
Mental-physical handicaps
Learning disability
Recurrence
Cranial nerve palsies
Raised ICP
Subdural effusion
Cerebral palsy
Hydrocephalus
Mental-physical handicaps
Learning disability
Recurrence
PREVENTIONS
Regular ANC check up
Treatment of infections during ANC period
Correction of anemiaand control of Gestational Diabetes
Training of local Daisor paramedics about proper delivery and referralsystem
Raising awareness about institutionaldelivery
Manage actively fetal distress
Ensuring proper training of neonatal resuscitations
Regular ANC check up
Treatment of infections during ANC period
Correction of anemiaand control of Gestational Diabetes
Training of local Daisor paramedics about proper delivery and referralsystem
Raising awareness about institutionaldelivery
Manage actively fetal distress
Ensuring proper training of neonatal resuscitations
MANAGEMENT
◦MEDICAL
◦GOALS
TO CONTROL CONVULSIONS
TO TREAT UNDERLYING PATHOLOGY
1.Initial stabilization
Establish TABC
Apply O2 and ventilations
Establish IV access
Take samples for initial studies
◦MEDICAL
◦GOALS
TO CONTROL CONVULSIONS
TO TREAT UNDERLYING PATHOLOGY
1.Initial stabilization
Establish TABC
Apply O2 and ventilations
Establish IV access
Take samples for initial studies
2. DRUGS
First line (benzodiazepines)
Diazepam-0.5mg/kg (max 10 mg) IV slow
Lorazepam-0.05-0.1mg/kg IV per rectum or sublingual
Midazolam-0.1-0.2mg/kg IV or IM
Dose may be repeated q5minutes up to 3 doses
Monitor respirations
First line (benzodiazepines)
Diazepam-0.5mg/kg (max 10 mg) IV slow
Lorazepam-0.05-0.1mg/kg IV per rectum or sublingual
Midazolam-0.1-0.2mg/kg IV or IM
Dose may be repeated q5minutes up to 3 doses
Monitor respirations
3. SECOND LINE DRUGS (PHENYTOIN AND BARBITURATES
Phenytoin-20mg/kg slow IV ( no faster than 1 mg/kg/min with a maximum
of 50 mg/min
Phenobarbitone-15-20 mg/kg slow IV
Monitor blood pressure
4. Other drugs
Carabamzepine-10-15mg/kg/day
Sodium valproate-20-60mg/kg/day
Felbamate-15mg/kg/day
Phenytoin-20mg/kg slow IV ( no faster than 1 mg/kg/min with a maximum
of 50 mg/min
Phenobarbitone-15-20 mg/kg slow IV
Monitor blood pressure
4. Other drugs
Carabamzepine-10-15mg/kg/day
Sodium valproate-20-60mg/kg/day
Felbamate-15mg/kg/day
Surgical management
Resectivesurgery
Callostomy
Multiple subpialtransection
Resectivesurgery
Callostomy
Multiple subpialtransection
BIBLIOGRAPHY
1.Pilliteri. A child health nursing, care of the child and fanmily. New
York: Lippincott willisamsand wilkins; 1999.P. 580-84
2.Dutta P. pediatric nursing. 2
nd
ed. New Delhi: Jaypeebrothers,
2009. P. 282-86
3.Jacob A. PaediatricNursing. 1
st
ed. Indore: NR Brothers; 1997.P.
257-263
1.Pilliteri. A child health nursing, care of the child and fanmily. New
York: Lippincott willisamsand wilkins; 1999.P. 580-84
2.Dutta P. pediatric nursing. 2
nd
ed. New Delhi: Jaypeebrothers,
2009. P. 282-86
3.Jacob A. PaediatricNursing. 1
st
ed. Indore: NR Brothers; 1997.P.
257-263
4. Marlow DR, Redding BA. Text book of pediatric nursing.
6
th
ed. New Delhi: Elseiver. 2011; P.947-56
5. GhaiP.O, Paul K.V, Bagg. A essential pediatrics. 7
th
ed.
New Delhi: CBS publishers; 2010.P. 1302-08
6
th
ed. New Delhi: Elseiver. 2011; P.947-56
5. GhaiP.O, Paul K.V, Bagg. A essential pediatrics. 7
th
ed.
New Delhi: CBS publishers; 2010.P. 1302-08
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