| Literature DB >> 33391282 |
Priyanka Madhav Kambli1, Umair Ahmed Bargir1, Reetika Malik Yadav1, Maya Ravishankar Gupta1, Aparna Dhondi Dalvi1, Gouri Hule1, Madhura Kelkar1, Sneha Sawant-Desai1, Priyanka Setia1, Neha Jodhawat1, Nayana Nambiar1, Amruta Dhawale1, Pallavi Gaikwad1, Shweta Shinde1, Prasad Taur2, Vijaya Gowri2, Ambreen Pandrowala3, Anju Gupta4, Vibhu Joshi4, Madhubala Sharma4, Kanika Arora4, Rakesh Kumar Pilania4, Himanshi Chaudhary4, Amita Agarwal5, Shobita Katiyar5, Sagar Bhattad6, Stalin Ramprakash7, Raghuram Cp7, Ananthvikas Jayaram8, Vinod Gornale9, Revathi Raj10, Ramya Uppuluri10, Meena Sivasankaran11, Deenadayalan Munirathnam11, Harsha Prasad Lashkari12, Manas Kalra13, Anupam Sachdeva13, Avinash Sharma14, Sarath Balaji15, Geeta Madathil Govindraj16, Sunil Karande17, Ruchi Nanavati18, Mamta Manglani19, Girish Subramanyam20, Abhilasha Sampagar21, Indumathi Ck22, Parinitha Gutha23, Swati Kanakia24, Shiv Prasad Mundada25, Vidya Krishna26, Sheela Nampoothiri27, Sandeep Nemani28, Amit Rawat4, Mukesh Desai2, Manisha Madkaikar1.
Abstract
Leukocyte adhesion deficiency (LAD) syndrome is a group of inborn errors of immunity characterized by a defect in the cascade of the activation and adhesion leading to the failure of leukocyte to migrate to the site of tissue injury. Three different types of LAD have been described. The most common subtype is LAD type 1 (LAD1) caused due to defects in the ITGβ2 gene. LAD type 2 (LAD2) is caused by mutations in the SLC35C1 gene leading to a generalized loss of expression of fucosylated glycans on the cell surface and LAD type 3 (LAD3) is caused by mutations in the FERMT3 gene resulting in platelet function defects along with immunodeficiency. There is a paucity of data available from India on LAD syndromes. The present study is a retrospective analysis of patients with LAD collated from 28 different centers across India. For LAD1, the diagnosis was based on clinical features and flow cytometric expression of CD18 on peripheral blood leukocytes and molecular confirmation by Sanger sequencing. For patients with LAD3 diagnosis was largely based on clinical manifestations and identification of the pathogenic mutation in the FERMT3 gene by next-generation Sequencing. Of the total 132 cases diagnosed with LAD, 127 were LAD1 and 5 were LAD3. The majority of our patients (83%) had CD18 expression less than 2% on neutrophils (LAD1°) and presented within the first three months of life with omphalitis, skin and soft tissue infections, delayed umbilical cord detachment, otitis media, and sepsis. The patients with CD18 expression of more than 30% (LAD1+) presented later in life with skin ulcers being the commonest manifestation. Bleeding manifestations were common in patients with LAD3. Persistent neutrophilic leukocytosis was the characteristic finding in all patients. 35 novel mutations were detected in the ITGβ2 gene, and 4 novel mutations were detected in the FERMT3 gene. The study thus presents one of the largest cohorts of patients from India with LAD, focusing on clinical features, immunological characteristics, and molecular spectrum.Entities:
Keywords: CD11; CD18; FERMT3; ITGβ2; Leukocyte Adhesion deficiency
Year: 2020 PMID: 33391282 PMCID: PMC7772426 DOI: 10.3389/fimmu.2020.612703
Source DB: PubMed Journal: Front Immunol ISSN: 1664-3224 Impact factor: 7.561