FANCA Gene Mutations with 8 Novel Molecular Changes in Indian Fanconi Anemia Patients

Solanki, Avani; Mohanty, Purvi; Shukla, Pallavi; Rao, Anita; Ghosh, Kanjaksha; Vundinti, Babu Rao

doi:10.1371/journal.pone.0147016

Cited by 18 publications

(27 citation statements)

References 24 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Out of these 26 mutations 7 were missense of which three(3/7;43%) were novel i.e., c.3679C>G (p.Ala1227Pro), c.1273C>G (p.Asp425His), c.3992T>C (p.Leu1331Pro) and (5/7; 57%) were already reported from Netherlands (AMEZIANE et al, 2008), Japan (TACHIBANA et al, 1999b;ADACHI et al, 2002;YAGASAKI et al, 2004b), Brazil (LEVRAN et al, 1997 and USA populations (CHANDRA et al, 2005a;LEVRAN et al, 2005b). The c.2851C>T mutation in exon 29 is highly predominant in India (SOLANKI et al, 2016), Netherlands (AMEZIANE et al, 2008, and USA (CHANDRA et al, 2005a;LEVRAN et al, 2005b). In addition, c.2574C>G mutation in exon 27 is highly prevalent in India (SOLANKI et al, 2016), Netherlands (WIJKER et al, 1999a), Israeli (TAMARY et al, 2000TAMARY et al, 2004a) populations and c.1303C>T in exon14 is highly dominant in India (SOLANKI et al, 2016), Japan (TACHIBANA et al, 1999b;ADACHI et al, 2002;YAGASAKI et al, 2004b), andBrazil (LEVRAN et al, 1997).…”

Section: Indiamentioning

confidence: 93%

“…The most common mutation was 2546delCin exon 27 which was present in six out of 15 patients (40%), resulting in a premature termination codon 40 codons downstream and formation of a truncated protein of 887 amino acids (TACHIBANA et al, 1999b). Among the other base substitutions, 1303C>T pathogenic missense mutation was found in 12 out of 15 analyzed FA patients (80%) and has reported higher incidence in Indian (SOLANKI et al, 2016) and Brazilian FA patients as well . Another report by Adachi and his group also described some FANCA mutations but those were previously reported by Levran et al, 2005) (see Table 1) (ADACHI et al, 2002).…”

Section: Japanmentioning

confidence: 99%

“…Most recently Solanki, et al (2016) studied 550-FA suspected adults and children (SOLANKI et al, 2016). After chromosomal breakage test, 61 confirmed cases with FA were subjected to MLPA analysis and direct sequencing.…”

Section: Indiamentioning

confidence: 99%

“…After chromosomal breakage test, 61 confirmed cases with FA were subjected to MLPA analysis and direct sequencing. A total of 26 FANCA variations were identified in 34 unrelated individual of which 8 were novel mutations and remaining were previously reported (SOLANKI et al,. 2016).…”

Section: Indiamentioning

confidence: 99%

“…The c.2851C>T mutation in exon 29 is highly predominant in India (SOLANKI et al, 2016), Netherlands (AMEZIANE et al, 2008, and USA (CHANDRA et al, 2005a;LEVRAN et al, 2005b). In addition, c.2574C>G mutation in exon 27 is highly prevalent in India (SOLANKI et al, 2016), Netherlands (WIJKER et al, 1999a), Israeli (TAMARY et al, 2000TAMARY et al, 2004a) populations and c.1303C>T in exon14 is highly dominant in India (SOLANKI et al, 2016), Japan (TACHIBANA et al, 1999b;ADACHI et al, 2002;YAGASAKI et al, 2004b), andBrazil (LEVRAN et al, 1997). Among 6 nonsense mutations identified in this study, 4 were new c.2182C>T, c.2630C>G, c.3189G>A and c.3677C>G in exon 24, 28, 32, 37 respectively.…”

Section: Indiamentioning

confidence: 99%

See 4 more Smart Citations

FANCA and contribution of studies from Asian populations to the understanding of fanca mediated Fanconi anemia

Shahid¹,

Firasat²

2019

Genetika

View full text Add to dashboard Cite

Section: Indiamentioning

confidence: 93%

Section: Japanmentioning

confidence: 99%

Section: Indiamentioning

confidence: 99%

Section: Indiamentioning

confidence: 99%

Section: Indiamentioning

confidence: 99%

See 3 more Smart Citations

FANCA and contribution of studies from Asian populations to the understanding of fanca mediated Fanconi anemia

Shahid¹,

Firasat²

2019

Genetika

View full text Add to dashboard Cite

Fanconi Anemia: Challenges in Diagnosis and Management—A Case Series Report

Eghbali,

Safdari,

Yousefi Roozbahani

et al. 2024

Clinical Case Reports

View full text Add to dashboard Cite

Fanconi anemia (FA) is a rare inherited disorder characterized by congenital abnormalities, progressive bone marrow failure, and a predisposition to malignancies. Detecting FA can be challenging, as it involves identifying increased chromosomal sensitivity to DNA cross‐linking agents and detecting causative genetic variants via genome sequencing. We report two cases of siblings with FA, both confirmed to have the FANCD2 variant through whole‐exome sequencing (WES). The first patient presented with epistaxis, petechiae, ecchymosis, and lower limb edema. The second patient exhibited epistaxis, diabetes, developmental delay, and physical abnormalities. Interestingly, both patients had negative results on the initial chromosomal breakage test with mitomycin C, a commonly used diagnostic tool for FA. However, further investigation with WES revealed the presence of the FANCD2 variant, confirming the FA diagnosis. This case report highlights the challenges in diagnosing FA, particularly when initial screening tests yield negative results. Molecular genetic testing, such as WES, can provide a definitive diagnosis and guide appropriate management strategies. Early and accurate diagnosis is crucial for improving outcomes in individuals with this potentially fatal illness, as promising advancements in treatments such as hematopoietic stem cell transplantation and gene therapy offer hope for addressing FA.

show abstract

A comprehensive molecular study identified 12 complementation groups with 56 novel FANC gene variants in Indian Fanconi anemia subjects

et al. 2021

Self Cite

View full text Add to dashboard Cite

Fanconi anemia (FA) is a rare autosomal or X-linked genetic disorder characterized by chromosomal breakages, congenital abnormalities, bone marrow failure (BMF), and cancer. There has been a discovery of 22 FANC genes known to be involved in the FA pathway. This wide number of pathway components makes molecular diagnosis challenging for FA. We present here the most comprehensive molecular diagnosis of FA subjects from India. We observed a high frequency (4.42 ± 1.5 breaks/metaphase) of chromosomal breakages in 181 FA subjects. The major clinical abnormalities observed were skin pigmentation (70.2%), short stature (46.4%), and skeletal abnormalities (43.1%), along with a few minor clinical abnormalities.

show abstract

FANCA Gene Mutations with 8 Novel Molecular Changes in Indian Fanconi Anemia Patients

Cited by 18 publications

References 24 publications

FANCA and contribution of studies from Asian populations to the understanding of fanca mediated Fanconi anemia

FANCA and contribution of studies from Asian populations to the understanding of fanca mediated Fanconi anemia

Fanconi Anemia: Challenges in Diagnosis and Management—A Case Series Report

A comprehensive molecular study identified 12 complementation groups with 56 novel FANC gene variants in Indian Fanconi anemia subjects

Contact Info

Product

Resources

About