Identification of HLA-A, HLA-B, and HLA-C triple homozygous and double homozygous donors: a path toward synthetic superdonor advanced therapeutic medicinal products

Daniel Naumovas; Barbara Valeria Rojas Araya; Catalina M Polanco; Victor Andrade; Rita Čekauskienė; Beatričė Valatkaitė-Rakštienė; Inga Laurinaitytė; Artūras Jakubauskas; Mindaugas Stoškus; Laimonas Griškevičius; Ivan Nalvarte; Jose Inzunza; Daiva Baltriukienė; Jonathan Arias

doi:10.3389/fimmu.2025.1626787

Title	Identification of HLA-A, HLA-B, and HLA-C triple homozygous and double homozygous donors: a path toward synthetic superdonor advanced therapeutic medicinal products
Authors	Naumovas, Daniel ; Rojas Araya, Barbara Valeria ; Polanco, Catalina M ; Andrade, Victor ; Čekauskienė, Rita ; Valatkaitė-Rakštienė, Beatričė ; Laurinaitytė, Inga ; Jakubauskas, Artūras ; Stoškus, Mindaugas ; Griškevičius, Laimonas ; Nalvarte, Ivan ; Inzunza, Jose ; Baltriukienė, Daiva ; Arias, Jonathan
DOI	10.3389/fimmu.2025.1626787
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Is Part of	Frontiers in immunology.. Lausanne : Frontiers Media SA. 2025, vol. 16, art. no. 1626787, p. [1-13].. eISSN 1664-3224
Keywords [eng]	superdonor ; HLA class I ; immune compatibility ; hypoimmunogenic ; population genetics
Abstract [eng]	Human-induced pluripotent stem cells with broad immune compatibility are highly desirable for regenerative medicine applications. Human leukocyte antigen (HLA) class I homozygous cell sources are ideal for immune compatibility modeling. Here, we profile HLA-A, HLA-B, and HLA-C alleles in 3,496 Lithuanian donors genotyped at three-field resolution. The five most frequent alleles constitute 74.6% of HLA-A, 43.2% of HLA-B, and 59.2% of HLA-C, with HLA-A02:01:01, HLA-B07:02:01, and HLA-C*07:02:01 being the most common. Lithuanian allele frequencies closely resemble those of European-American and British populations. We identified 153 double homozygotes and 51 triple homozygotes for HLA-A, HLA-B, and HLA-C. Compatibility modeling showed that triple homozygous profiles match 60.5% of Lithuanians, 13.4% of the British population, and 7.4% of European-Americans. CRISPR-Cas9 guide RNA design yielded 54 candidates predicted to disrupt HLA-A or HLA-B while preserving HLA-C, producing edited profiles matching over 97.9% of Lithuanians, 95.7% of European-Americans, and 95.5% of the British population. Finally, we established 15 fibroblast lines from triple homozygotes as a bioresource for the derivation of human-induced pluripotent stem cells and immune compatibility studies.
Published	Lausanne : Frontiers Media SA
Type	Journal article
Language	English
Publication date	2025
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„Identification of HLA-A, HLA-B, and HLA-C triple homozygous and double homozygous donors: a path toward synthetic superdonor advanced therapeutic medicinal products“