Published online Feb 26, 2019. doi: 10.12998/wjcc.v7.i4.494
Peer-review started: November 20, 2018
First decision: December 20, 2018
Revised: January 16, 2019
Accepted: January 29, 2019
Article in press: January 30, 2019
Published online: February 26, 2019
Pediatric recurrent acute liver failure (RALF) with recovery between episodes is rare. Causes include autoimmune disease, which may flare and subside; intermittent exposure to toxins, as with ingestions; and metabolic disorders, among them the fever-associated crises ascribed to biallelic mutations in SCYL1, with RALF beginning in infancy. SCYL1 disease manifest with RALF, as known to date, includes central and peripheral neurologic and muscular morbidity (hepatocerebellar neuropathy syndrome). Primary ventilatory and skeletal diseases also have been noted in some reports.
We describe a Han Chinese boy in whom fever-associated RALF began at age 14 mo. Bilateral femoral head abnormalities and mild impairment of neurologic function were first noted aged 8 years 6 mo. Liver biopsy after the third RALF episode (7 years) and during resolution of the fourth RALF episode (8 years 6 mo) found abnormal architecture and hepatic fibrosis, respectively. Whole-exome sequencing revealed homozygosity for the novel frameshift mutation c.92_93insGGGCCCT, p.(H32Gfs*20) in SCYL1 (parental heterozygosity confirmed).
Our findings expand the mutational and clinical spectrum of SCYL1 disease. In our patient a substantial neurologic component was lacking and skeletal disease was identified relatively late.
Core tip: An infant or child with recurrent acute liver failure may have biallelic mutation in SCYL1. A search for causes should include evaluation of this gene even if neurologic or skeletal disease is not appreciated.
- Citation: Li JQ, Gong JY, Knisely AS, Zhang MH, Wang JS. Recurrent acute liver failure associated with novel SCYL1 mutation: A case report. World J Clin Cases 2019; 7(4): 494-499
- URL: https://www.wjgnet.com/2307-8960/full/v7/i4/494.htm
- DOI: https://dx.doi.org/10.12998/wjcc.v7.i4.494
An unusual form of acute liver failure (ALF) occurs in children. Starting in infancy, episodes of hepatic insufficiency recur. These episodes may be preceded by fever (and thus be ascribed to antipyretics, in particular paracetamol)[1-3]. They may not be restricted to childhood[4,5] and may be fatal[6]. They are characterized by clinical-laboratory findings that include marked elevations in serum transaminase activity, severe coagulopathy, conjugated hyperbilirubinemia, and normal or only slightly elevated serum gamma-glutamyl transpeptidase activity[2,4]. Hepatic crises, with less severe injury, also are seen[1-5]. The causes of recurrent ALF (RALF), as this disorder is termed, are incompletely understood, although instances have been ascribed to biallelic mutation in SCYL1 (MIM: 607982)[7] or NBAS (MIM: 608025)[4]. NBAS disease is multisystem in some patients[3,6,8] and manifest only as RALF in others[2,4]. The few patients yet reported with SCYL1 disease have exhibited isolated RALF in conjunction with a range of mild to more marked neurological phenotypes, including spinocerebellar ataxia and neurodegeneration[7,9-11]. In one, recurrent ventilatory failure was clinically prominent; RALF was not described[12].
We report a novel homozygous mutation in SCYL1 in a Han Chinese boy who had RALF with onset in infancy and in whom, aged 8 years 6 mo, mild neurologic dysfunction and bilateral femoral head abnormalities were identified. Our observations expand the clinical and mutational spectrum of SCYL1 disease.
A 7-year-old boy was admitted to our hospital due to recurrent episodes of ALF.
The patient was well till age 14 mo, when a fever was treated with the non-steroidal anti-inflammatory agent nimesulide. Jaundice developed, with elevated transaminase activity. Injury fell short of frank ALF, constituting instead a “liver crisis”. Two episodes of ALF followed at ages of 3 years 6 mo and 6 years 3 mo (Table 1). Clinical, laboratory, and imaging-study findings between episodes were normal. At the age of 7 years, shortly after his third RALF episode, he was referred to our hospital for etiological diagnosis.
| Age 3 y 6 mo | Age 6 y 3 mo | Age 8 y 5mo | Range | |
| Febrile illness before ALF | Yes | Yes | Yes | |
| Using antipyretics before ALF | Yes | No | Yes | |
| Duration | > 4 mo | > 1 mo | > 1 mo | |
| Max TB (μmol/L) | 504.0 | 305.7 | 554.0 | 5.1-17.1 |
| Max DB (μmol/L) | 288.0 | 125.0 | 264.7 | 0-6.0 |
| Max ALT (IU/L) | 414 | 1865 | 881 | 0-40 |
| Max AST (IU/L) | 2050 | 4900 | 1648 | 15-60 |
| Max GGT (IU/L) | 117 | 39 | 70 | 7-50 |
| Max PT (s) | 24.9 | 29.5 | 26.7 | 11.0-14.5 |
| Hepatomegaly | Yes | Yes | Yes | |
| Splenomegaly | No | No | Yes | |
| Additional features | Antipyretic- induced hepatopathy diagnosed | Multi-organ involvement1 | Multi-organ involvement2 |
His parents and he denied any history of disease beyond that summarized above.
He was born at term (weight 3 kg) by elective cesarean section after an uncomplicated pregnancy. He is the second child of a Han Chinese couple who deny consanguinity. His sibling, a brother, is well.
Physical examination on admission found no abnormalities.
Blood, urine, and stool routine test results, viral serological markers (hepatotropic viruses, Epstein-Barr virus, cytomegalovirus, and human immunodeficiency virus 1), biomarkers of toxoplasma infection, of thyroid function, and of hepatobiliary injury, and values for cholesterol, triglycerides, creatine phosphokinase, glucose, ceruloplasmin, blood lactate, blood ammonia, carbonyldiamide, creatinine, uric acid, urine organic acids, alpha-fetoprotein, and immunoglobulin levels were unremarkable. The value of 25-(OH)D3 was 13.69 ng/mL (normal: 30-100 ng/mL).
Cranial magnetic resonance imaging showed a cyst (90 mm × 30 mm) in the cisterna magna and a relatively small cerebellum. The optic nerves were normal. Abdominal ultrasonography and echocardiography showed no significant abnormalities.
Findings on ophthalmologic evaluation were unremarkable. Liver biopsy found mildly abnormal architecture, without fibrosis, in a pattern suggesting disordered perfusion; no ultrastructural abnormalities were apparent. The Denver developmental screening test, which covers gross motor, language, fine motor-adaptive, and personal-social skills[13], found a low developmental quotient (< 47, normal > 70) and mental index (63, normal > 70).
With the approval of the ethics committee of the Jinshan Hospital of Fudan University (Jinyi Lunli Keyan-2014-13-01) and after obtaining written informed consent from the parents of the patient, DNA was isolated from peripheral blood samples obtained from the proband, his brother, and his parents. Whole-exome sequencing was conducted as described[2] (Genesky Biotechnologies, Shanghai, China). Exomes were captured using a SureSelectXT Human All Exon V6 kit (Agilent Technologies, Foster, CA). Sequencing (250 bp paired-end reads) was performed using the Illumina hiseq2500 platform following the manufacturer’s instructions (Illumina, San Diego, CA). Burrows-Wheeler Aligner software (http://bio-bwa.sourceforge.net/) was used for read alignment (hg19; NCBI build 37; February, 2009). Variant calling was performed with Varscan (http://varscan.sourceforge.net/) and GATK Haplotype-Caller (https://software.broadinstitute.org/gatk/best-practices/). Mean coverage of the exome was 140× with 91% of the exome covered at least 10 times and 80% covered at greater than 20×. The proband’s variants were filtered for minor allele frequency < 1% against Thousand Genomes Project (http://www.1000genomes.org/home), NHLBI Exome Sequencing Project (http://evs.gs.washington.edu/EVS/), Exome Aggregation Consortium Server (http://exac.broadinstitute.org/), and Genesky in-house databases. Variants in ALF-associated genes (Supplementary file 1) assessed by SIFT (http://sift.jcvi.org/), Polyphen-2 (http://genetics.bwh.harvard.edu/pph2/), or MutationTaster[14] (http://www.mutationtaster.org/) as pathogenic and present in accord with inheritance modes were considered of interest. Sanger sequencing was used to confirm variants in the proband and to seek them in his parents and brother.
The homozygous mutation c.92_93insGGGCCCT, p.(H32Gfs*20) in exon 1 in SCYL1 (NM_020680) was identified in the proband. His brother did not harbor this mutation. Each of their parents was heterozygous for the mutation, consistent with recessive inheritance. The mutation detected by exome sequencing was again identified on Sanger sequencing (Supplementary file 2). No other variant of interest was identified in any ALF-associated gene. The insertion of GGGCCCT between nucleotides 92 and 93 within exon 1 is predicted to result in the substitution of 19 abnormal amino acid residues (His32-Val50), followed by a stop codon at codon 51. MutationTaster predicts that this results in nonsense-mediated mRNA decay[14]. The variant is novel; it was not recorded in Exome Aggregation Consortium Server, NHLBI Exome Sequencing Project, Thousand Genomes Project, or Genesky in-house databases.
SCYL1 disease.
Supportive care during episodes of ALF or crises followed accepted guidelines and was not specific for any particular form of hepatic dysfunction. They included antibiotics to resist bacterial infection, ”liver protectant drugs” (D-glucurono-3,6-lactone, diammonium glycyrrhizinate, polyene phosphatidylcholine, etc.), cholagogues and choleretics (ursodeoxycholic acid, cholestyramine, etc.), prednisone, and supplementary fat-soluble vitamins A, D, E, and K.
The patient had his fourth episode of RALF at 8 years 5 mo (Table 1). During resolution of this episode, liver biopsy was conducted again. Alanine transaminase and aspartate aminotransferase values 2 d before liver biopsy were 91 IU/L (expected: 0-40 IU/L) and 476 IU/L (normal: 15-60 IU/L). Ballooning change of hepatocytes, some with cytoplasmic bile pigment, and hepatic fibrosis were observed. A comprehensive skeletal survey by radionuclide bone scan showed bilateral hip joint widening and bilateral femoral head flattening highly suggestive of bilateral femoral head necrosis. The patient failed finger-to-nose testing and Romberg testing, indicating cerebellar ataxia. However, muscle strength, muscular tension, stretch reflexes, deep sensory perception, and motor function were normal. At last evaluation, aged 8 years 7 mo, biomarker values in the proband were normal.
SCYL1 encodes a kinase-like protein in the SCY1-like family[15,16]. SCYL1 may function as a scaffolding protein, involved in Golgi-to-endoplasmic reticulum retrograde transport and in Golgi integrity[17-19]. SCYL1 also acts in nucleocytoplasmic shuttling of tRNAs[20]. Biallelic mutations in SCYL1 were first identified in 2015 as an important cause of a hepatocerebellar neuropathy syndrome (spinocerebellar ataxia, autosomal recessive 21; MIM:616719)[7].
To date, only 5 reports have described 14 patients harboring homozygous or compound heterozygous mutations in SCYL1[7,9-12]. Thirteen patients had similar hepatic features[7,9-11]; in the 14th, features of liver disease were present, but recurrent ventilatory failure dominated clinical illness[12]. Neurologic phenotypes varied, including peripheral neuropathy, ataxia, tremor, stuttering, speech-development delay, intellectual disability, microcephaly, and abnormal intracranial magnetic-resonance imaging findings. Six SCYL1-deficient patients had cerebellar atrophy and 2 siblings had optic nerve thinning[7,10,12].
Our patient had a classic hepatic phenotype, with one episode of liver crisis (aged 14 mo) and 3 episodes of acute liver failure (aged 3 years 6 mo, 6 years 3 mo, and 8 years 5 mo). Each episode was preceded by a febrile illness. Hepatobiliary-injury biomarker values recovered completely between episodes. Not all episodes of febrile illness led to hepatic crisis. Liver biopsy conducted after the third RALF episode (7 years) and during resolution of the fourth RALF episode (8 years 6 mo) revealed slightly abnormal architecture and hepatic fibrosis, respectively.
In our patient, relative cerebellar hypoplasia may be secondary to the cyst in the cisterna magna; vermis atrophy was not identified, and optic nerves were not thinned. Clinical neurologic features are at this writing minimal, with low developmental quotient and mental index, minor intracranial abnormalities, and abnormal coordination tests. These may worsen as the patient ages, or other abnormalities may yet declare themselves. Neurologic abnormalities usually are noted in SCYL1 disease after liver disease has appeared (Supplementary file 3). To evaluate SCLY1 in infants or children with RALF thus is indicated even if neurologic disease is inapparent. Long-term follow-up is necessary for best correlation between mutation and phenotypic consequences.
Worth noting is that skeletal abnormalities were observed in 8 of 14 SCYL1-deficiency patients. Skeletal phenotypes varied, including short stature, hip dysplasia, coronal clefting of ribs, scoliosis, lumbar lordosis, and thoracic vertebral abnormalities[9-11]. Our patient had bilateral femoral head disease, not reported before in association with SCYL1 mutation. At least some of the skeletal abnormalities described appear primary rather than resulting from neuromuscular dysfunction, suggesting that such abnormalities may be an important clinical manifestation of SCYL1 disease. Systemic skeletal examinations thus may be essential for children with SCYL1 deficiency.
Early identification of the cause of ALF is fundamental for disease-specific management. In our patient, assignment of diagnosis to mutation in a specific gene shifted the context in which we viewed his findings on examination, changing our expectations for the course of what now can be considered as a multisystem disorder. For instance, during the fourth RALF episode, after genetic diagnosis, a comprehensive skeletal survey and more detailed neurologic examination were performed. Our care has become better focused and, with the progress of the disease, may perhaps permit orthopedic, physiatric, and neurologic intervention for directed support. In addition, genetic diagnosis can also help in prenatal screening.
Our patient is the first East Asian described with SCYL1-associated RALF. The SCYL1 mutation c.92_93insGGGCCCT, p.(H32Gfs*20), which he harbors in homozygous state, is predicted to result in nonsense-mediated decay of a prematurely terminated RNA transcript. Although we lack direct evidence for lack of SCYL1 expression in our patient, we thus consider him the 15th identified patient with RALF due to SCYL1 disease. We call attention to his clinical phenotype, with scant neurologic dysfunction identified thus far and relatively late-onset skeletal disease, although our findings are – without life-long follow-up – necessarily incomplete. We suggest that even if neurologic features of disease are few (“atypical” SCYL1 disease), SCYL1 defects should be considered as possibly underlying early-onset fever-related RALF. We also note as deserving further study the association between skeletal abnormalities and SCYL1 disease.
Even if neurologic features of disease are few, SCYL1 defects should be considered as possibly underlying early-onset fever-related RALF. Systemic skeletal examinations are in order for children with SCYL1 deficiency.
The authors are grateful for the support of the patient’s family and thank referring physicians, nurses, and technical staff.
Manuscript source: Unsolicited manuscript
Specialty type: Medicine, research and experimental
Country of origin: China
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P- Reviewer: Chatzigeorgiou A, Nacif LS, Zheng YW S- Editor: Wang JL L- Editor: Wang TQ E- Editor: Tan WW
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