Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UMLS:C0017160 (
gastroenteritis
)
11,398
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Mutations in
PRRT2
genes have been identified as a major cause of benign infantile epilepsy and/or paroxysmal kinesigenic dyskinesia. We explored mutations in
PRRT2
in Japanese patients with BIE as well as its related conditions including convulsion with mild
gastroenteritis
and benign early infantile epilepsy. We explored
PRRT2
mutations in Japanese children who had had unprovoked infantile seizures or convulsion with mild
gastroenteritis
. The probands included 16 children with benign infantile epilepsy, 6 children with convulsions with mild
gastroenteritis
, and 2 siblings with benign early infantile epilepsy. In addition, we recruited samples from family members when
PRRT2
mutation was identified in the proband. Statistical analyses were performed to identify differences in probands with benign infantile epilepsy according to the presence or absence of
PRRT2
mutation. Among a total of 24 probands,
PRRT2
mutations was identified only in 6 probands with benign infantile epilepsy. A common insertion mutation, c.649_650insC, was found in 5 families and a novel missense mutation, c.981C>G (I327M), in one. The family history of paroxysmal kinesigenic dyskinesia was more common in probands with
PRRT2
mutations than in those without mutations. Our study revealed that
PRRT2
mutations are common in Japanese patients with benign infantile epilepsy, especially in patients with a family history of paroxysmal kinesigenic dyskinesia.
...
PMID:PRRT2 mutation in Japanese children with benign infantile epilepsy. 2313 49
Background:
Non-febrile illness seizures may present in previously healthy children as afebrile seizures associated with minor infections, such as mild
gastroenteritis
or respiratory tract infections, and are linked to a genetic predisposition. For the novel human coronavirus SARS-CoV-2, causing COVID-19, fever, cough, and gastrointestinal complaints are the most common symptoms in children, and a hyperimmune response may be present. No detailed temporally associated neurological complications have been documented in pediatric case series so far.
Case description:
We present the case of a 3-months-old girl with non-febrile repeated seizures in a COVID-19 family setting. The infant started with a mild fever and cough that lasted for 2 days. At day 6 from onset, the girl presented with two focal motor seizures with impaired consciousness and awareness. All investigations ruled out signs of meningo-encephalitis or active epilepsy, including normal electroencephalogram and cerebral magnetic resonance imaging. PCR from nasal and throat swabs was positive for SARS-CoV-2. Remarkably, blood ferritin and D-dimer levels were increased. At day 9, the infant presented another afebrile motor seizure, and levetiracetam dose was modified there was a favorable response within 3 months of the follow-up. Much interest has been raised with regards to host genetic determinants to disease severity and susceptibility to COVID-19. We thus performed whole exome sequencing, revealing a pathogenic frameshift mutation in the
PRRT2
gene in both the mother and the infant. The mother had presented two late infantile febrile convulsions with normal outcome afterwards.
Discussion:
The hyperimmune response described in adult cases with COVID-19 can be seen in infants, even in the absence of respiratory symptoms. Moreover, COVID-19 may present in infants as non-febrile seizures, triggering early onset seizures in infants with a genetic predisposition. In this pandemic situation, precision medicine using massive sequencing can shed light on underlying molecular mechanisms driving the host response to COVID-19.
...
PMID:Case Report: Benign Infantile Seizures Temporally Associated With COVID-19. 3285 May 63
