The Genetics of Sudden Infant Death Syndrome—Towards a Gene Reference Resource

Johannsen, Emma B; Baughn, Linda B.; Sharma, Neeraj; Zjacic, Nicolina; Pirooznia, Mehdi; Elhaik, Eran

doi:10.3390/genes12020216

Cited by 6 publications

(5 citation statements)

References 86 publications

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“…A common feature of all these disorders (except the short or sometimes medium chain) is fasting hypoketotic hypoglycemia [ 8 , 9 ]. Approximately 5% of sudden deaths in childhood are secondary to FAODs [ 10 ], most of which are diagnosed postmortem. With the implementation of newborn screening, the clinical presentation and its natural history have changed significantly.…”

Section: Introductionmentioning

confidence: 99%

Biochemical Markers for the Diagnosis of Mitochondrial Fatty Acid Oxidation Diseases

Ruíz-Sala

Quintana

2021

JCM

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Mitochondrial fatty acid β-oxidation (FAO) contributes a large proportion to the body’s energy needs in fasting and in situations of metabolic stress. Most tissues use energy from fatty acids, particularly the heart, skeletal muscle and the liver. In the brain, ketone bodies formed from FAO in the liver are used as the main source of energy. The mitochondrial fatty acid oxidation disorders (FAODs), which include the carnitine system defects, constitute a group of diseases with several types and subtypes and with variable clinical spectrum and prognosis, from paucisymptomatic cases to more severe affectations, with a 5% rate of sudden death in childhood, and with fasting hypoketotic hypoglycemia frequently occurring. The implementation of newborn screening programs has resulted in new challenges in diagnosis, with the detection of new phenotypes as well as carriers and false positive cases. In this article, a review of the biochemical markers used for the diagnosis of FAODs is presented. The analysis of acylcarnitines by MS/MS contributes to improving the biochemical diagnosis, both in affected patients and in newborn screening, but acylglycines, organic acids, and other metabolites are also reported. Moreover, this review recommends caution, and outlines the differences in the interpretation of the biomarkers depending on age, clinical situation and types of samples or techniques.

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Section: Introductionmentioning

confidence: 99%

Biochemical Markers for the Diagnosis of Mitochondrial Fatty Acid Oxidation Diseases

Ruíz-Sala

Quintana

2021

JCM

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“…SIDS/SUID risk is still likely defined by multifactorial genetic and environmental interactions [23,24]. In one of such subjects, we detected the missense mutation in PHOX2B.…”

Section: Plos Onementioning

confidence: 99%

Non-polyalanine repeat mutation in PHOX2B is detected in autopsy cases of sudden unexpected infant death

et al. 2022

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Background Congenital central hypoventilation syndrome (CCHS), which is caused by PHOX2B with phenotypic variations, has a point of controversy: CCHS is putatively involved in autopsy cases of sudden unexpected infant death (SUID) including sudden infant death syndrome. Objective The relation of CCHS to SUID cases was investigated by extensive genotyping of PHOX2B. Methods We analyzed 93 DNA samples of less than one-year-old SUID cases that were autopsied in our department. Unrelated adult volunteers (n = 942) were used as the control. Results No polyalanine tract expansion was detected in the SUID cases. The allelic frequencies of repeat contractions and SNP (rs28647582) in intron 2 were not significantly different from that in those control group. Further extensive sequencing revealed a non-polyalanine repeat mutation (NPARM) of c.905A>C in a sudden death case of a one-month-old male infant. This missense mutation (p.Asn302Thr), registered as rs779068107, was annotated to ‘Affected status is unknown’, but it might be associated with the sudden death. Conclusion NPARM was more plausibly related to sudden unexpected death than expansions because of severe clinical complications. This finding indicates possible CCHS involvement in forensic autopsy cases without ante-mortem diagnosis.

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“…Studies have shown that, compared to controls, SIDS children have more frequent significant abnormalities of both the serotonin transporter gene [17,18] and the monoamine oxidase gene [19,20], leading to decreased serotonergic receptor binding and reduced serotonin and tryptophan hydroxylase 2 levels in the brainstem with poor function of the autonomic nervous system. Moreover, alterations in genes encoding for cardiac ion channels [21,22], proteins involved in myocardial conduction [23], skeletal muscle sodium channels [24], several immune components (complement component C4, interleukin-10 promoter) [25,26], and heat shock proteins [27] have been reported. All of these findings suggest that SIDS prone children have significant differences in several body functions with poor response in front of lifethreatening conditions.…”

Section: Present Hypothesis On Sudden Infant Death Syndrome (Sids) De...mentioning

confidence: 99%

Home Cardiorespiratory Monitoring in Infants at Risk for Sudden Infant Death Syndrome (SIDS), Apparent Life-Threatening Event (ALTE) or Brief Resolved Unexplained Event (BRUE)

Sodini

Paglialonga

Antoniol

et al. 2022

Life

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Sudden infant death syndrome (SIDS) is defined as the sudden death of an infant younger than one year of age which remains unexplained after a thorough case investigation, including performance of a complete autopsy, examination of the death scene, and review of the clinical history. About 90% of SIDS occur before six months of age, the peak incidence is between two and four months, and the median age for death is elven weeks. The clinical, social, and economic relevance of SIDS, together with the evidence that prevention of this syndrome was possible, has significantly stimulated research into risk factors for the development of SIDS in the hope of being able to introduce new effective preventive measures. This narrative review discusses the potential relationships between apparent life-threatening events (ALTE) or brief resolved unexplained events (BRUE) and SIDS development, and when a home cardiorespiratory monitor is useful for prevention of these conditions. A literature analysis showed that home cardiorespiratory monitoring has been considered a potential method to identify not only ALTE and BRUE but SIDS also. ALTE and BRUE are generally due to underlying conditions that are not detectable in SIDS infants. A true relationship between these conditions has never been demonstrated. Use of home cardiorespiratory monitor is not recommended for SIDS, whereas it could be suggested for children with previous ALTE or severe BRUE or who are at risk of the development of these conditions. However, use of home cardiorespiratory monitors assumes that family members know the advantages and limitations of these devices after adequate education and instruction in their use.

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The Genetics of Sudden Infant Death Syndrome—Towards a Gene Reference Resource

Cited by 6 publications

References 86 publications

Biochemical Markers for the Diagnosis of Mitochondrial Fatty Acid Oxidation Diseases

Biochemical Markers for the Diagnosis of Mitochondrial Fatty Acid Oxidation Diseases

Non-polyalanine repeat mutation in PHOX2B is detected in autopsy cases of sudden unexpected infant death

Home Cardiorespiratory Monitoring in Infants at Risk for Sudden Infant Death Syndrome (SIDS), Apparent Life-Threatening Event (ALTE) or Brief Resolved Unexplained Event (BRUE)

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