Current Topics of Relevance to the Xenotransplantation of Free Pig Islets

Abstract

Pig islet xenotransplantation is a potential treatment for patients with type 1 diabetes. Current efforts are focused on identifying the optimal pig islet source and overcoming the immunological barrier. The optimal age of the pig donors remains controversial since both adult and neonatal pig islets have advantages. Isolation of adult islets using GMP grade collagenase has significantly improved the quantity and quality of adult islets, but neonatal islets can be isolated at a much lower cost. Certain culture media and coculture with mesenchymal stromal cells facilitate neonatal islet maturation and function. Genetic modification in pigs affords a promising strategy to prevent rejection. Deletion of expression of the three known carbohydrate xenoantigens (Gal, Neu5Gc, Sda) will certainly be beneficial in pig organ transplantation in humans, but this is not yet proven in islet transplantation, though the challenge of the ‘4th xenoantigen’ may prove problematic in nonhuman primate models. Blockade of the CD40/CD154 costimulation pathway leads to long-term islet graft survival (of up to 965 days). Anti-CD40mAbs have already been applied in phase II clinical trials of islet allotransplantation. Fc region-modified anti-CD154mAbs successfully prevent the thrombotic complications reported previously. In this review, we discuss (I) the optimal age of the islet-source pig, (ii) progress in genetic modification of pigs, (iii) the immunosuppressive regimen for pig islet xenotransplantation, and (iv) the reduction in the instant blood-mediated inflammatory reaction.

Introduction

Type 1 diabetes (T1D) is a chronic autoimmune disease characterized by pancreatic islet cell destruction by CD4⁺ and CD8⁺ T cells and autoantibodies, resulting in insulin deficiency and hyperglycemia (1). Conventional treatment of T1D includes exogenous insulin therapy, which reduces, but may not prevent, the development of the long-term complications of hyperglycemia. In late-stage T1D patients, especially those with ‘brittle’ diabetes, it is difficult to prevent complications such as cardiovascular disease, retinopathy, nephropathy, and life-threatening hypoglycemic episodes (1).

Islet allotransplantation has been identified as an efficient therapy for T1D, but, faced with the shortage of pancreases from deceased human donors, pig-to-human islet xenotransplantation has emerged as a potential alternative (2). Although pig-to-nonhuman primate (NHP) islet xenotransplantation has resulted in insulin independence, several problems remain.

The age of the islet-source pig may be important to islet quality. Adult pigs have a mature islet structure, lower galactose-α1,3-galactose (Gal) expression on islets, and a higher islet yield (3). Neonatal pig islets are easier to isolate and at a lower cost (3). To overcome immunological rejection of pig-to-NHP islet transplants, genetic modification of the source pig plays an important role by deleting xenoantigen expression and introducing human ‘protective’ proteins (4). New alternative modifications, e.g., expression of programmed cell death ligand 1 (PD-L1), are being explored. A consensus has been reached that, in regard to the transplantation of pig organs into humans, the expression of the three known carbohydrate xenoantigens (Gal, Neu5Gc, Sda) should be deleted (resulting in triple-knockout [TKO] pigs) (4, 5), but this remains uncertain after pig islet transplantation. However, there is a limitation in the TKO pig-to-NHP model because of the problem of the ‘4th xenoantigen’.

The selection of the immunosuppressive regimen plays a critical role in preventing the adaptive immune response (6). Although conventional immunosuppressive regimens are inefficient in preventing the adaptive response to pig cells, blockade of the CD40/CD154 costimulation pathway is successful, and has resulted in insulin-independence for a maximum of 965 days) (7). Emerging Fc region-modified anti-CD154mAbs successfully prevent the thrombotic complications seen previously (8, 9). Although anti-CD154 agents may be preferable, anti-CD40mAbs have already been applied in phase II clinical trials of human kidney allotransplantation (10).

In this review, we consider (i) the optimal age of the islet-source pig, (ii) the potential of genetic modification of the pig, (iii) the selection of the immunosuppressive regimen for pig-to-primate islet xenotransplantation, and (iv) potential steps to reduce the instant blood-mediated inflammatory reaction (IBMIR). We also briefly discuss the possible directions for future research.

Donor Age

Based on previous studies of pig-to-NHP islet xenotransplantation, pigs can be divided into three age groups: adult (>12 weeks), neonatal (~first 14 days after birth), and fetal. Their characteristics are summarized in Table 1. As fetal pig islets are not currently considered ideal sources for xenotransplantation due to defects in β-cell yield and immunogenicity, we will focus on adult and neonatal pigs.

Adult Pig Islets

To date, adult pig islets transplanted into NHPs have displayed the longest survival time (965 days) and have always been considered the primary source for islet xenotransplantation due to their superior islet yield, immediate insulin response, lower Gal expression, and higher β-cell percentage compared with neonatal pigs (Table 1). Female adult pigs that have produced >2 litters (retired breeders, usually >2 years old and > 200 kg) are preferred over young adult pigs because they consistently provide a higher yield of high-quality islets (3, 11). We add the ref: Bottino R, 2007 Our previous review summarized the above advantages (3). Using GMP-grade collagenase (collagenase AF-1 and liberase MTF C/T), one adult pig can yield up to 720,000IEQ (12), which is enough for islet xenotransplantation in a diabetic patient of approximately 60kg in weight. However, the limitations of adult pig islets include difficulty in isolation, higher costs for pig maintenance and islet isolation, and poor proliferative capacity (3) (Table 1).

Neonatal Islet Cell Clusters (NICC)

There have been only a few reports using NICC for transplantation into NHPs, with the longest survival being 260 days (13–16). The advantages of NICCs include (I) the need for only a short period of pig maintenance after birth, thus reducing the costs, (ii) easier isolation, thus increasing success and reducing isolation cost ($0.02/IEQ) compared to adult pig islets ($0.09/IEQ) (17), and (iii) greater proliferative capacity (3). However, there are some limitations. First, NICCs must be cultured to reaggregate the islet cluster before transplantation, although various modified culture media, the addition of growth factors, and coculture with mesenchymal stromal cells facilitate NICC islet maturation and function (18–21). Second, there is a delay in the in vivo response to glucose after transplantation (that may be >4 weeks in NHPs), and so measuring islet loss is difficult (3).

The difference in the glucose-stimulated insulin secretion index between adult pig islets and NICC remains controversial. Some research has indicated that NICC has a significantly higher stimulation index (4.7± 0.58) than adult pig islets (1.75 ± 0.60) (17), but other studies show the opposite (summarized in Table 2) (12, 17, 21–23). Therefore, the glucose-stimulated insulin secretion of adult pig islets and NICC may be equivalent.

In summary, a consensus on the optimal age for pig islet xenotransplantation has not been reached. Adult pig islets should be the primary option as better results have been achieved following transplantation into NHPs, but NICCs are regarded as a promising alternative islet source with several significant superiorities.

Gene Modification

The development of CRISPR/Cas9, an efficient genome editing technique, provides the capacity to produce pigs with multiple genetic modifications for xenotransplantation (Table 3) (24–41). We will here mainly focus on gene modification targets for carbohydrate xenoantigens and cellular immune response-related genes.

Carbohydrate Xenoantigen Genes

A consensus has been reached that the three known carbohydrate xenoantigen genes (Gal, Neu5Gc, Sda) should be knocked-out for pig-to-human organ transplantation (Table 4), but this is not ideal for pig-to-NHP organ transplantation because of the problems associated with the ‘4th xenoantigen’ (discussed in 42–46). It is well-known that pig organ grafts from CMAHKO pigs are associated with increased NHP IgM and IgG binding and serum complement-mediated cytotoxicity, resulting in acute xenograft rejection (42–46).

To our knowledge, the transplantation of TKO pig islets into NHPs has not been reported, and it remains unknown whether the ‘4^th xenoantigen’ is exposed in TKO pig islets as it is in vascular endothelial cells. Whether TKO islets would provide an advantage in this regard remains uncertain.

Of relevance to this point, there were no statistically significant differences in human IgM and IgG binding to isolated islet cells from GTKO/hCD46 and GTKO/hCD46/NeuGcKO pigs (47). Knockout of CMAH may therefore possibly have a different effect in islets than in solid organs. In one report, GTKO/CMAHKO pigs developed pathological features that are similar to those seen in anemia, possibly associated with variations in glycosylation on the red blood cell membranes of these pigs (48). Obukhova et al. have reviewed CMAH comprehensively (49).

If neonatal pigs are the source of islets (i.e., NICCs), in which expression of Gal is considerable, the deletion of expression of Gal (and possibly of Neu5Gc and Sda) will be advantageous.

Differences in N- and O-glycan profiles between human and porcine islets might prove to be the next gene modification sites. Novel xenoantigens include complex-type N-glycans with terminal neuraminic acid residues and high-mannose-type N-glycans with core fucosylation (50). Carbohydrate antigen microarrays in pigs and cynomolgus monkeys have revealed natural non-αGal antigens (e.g., Tn antigen, T antigen, GM2 glycolipid) and novel carbohydrate structures (e.g., Galβ1-4GlcNAcβ1-3Galβ1 and N-linked glycans with Manα1-6 (GlcNAcβ1-2Manα1-3)Manβ1-4GlcNAcβ) that are responsible for the IgM and IgG anti-carbohydrate antibody responses (51, 52). These findings suggest future gene modification sites to eliminate anti-carbohydrate antibody responses in pig-to-primate islet xenotransplantation.

For future studies of the 4th xenoantigen(s), several sources might be helpful, e.g., the database of Glycomics (http://www.functionalglycomics.org/). The National Center for Functional Glycomics (NCFG) (https://ncfg.hms.harvard.edu/) offers a CFG mammalian-type glycan microarray, with 600 glycans present, that might be helpful in studying xenoantigens in the future.

Cellular Immune Response-Related Genes

Progress in gene modification aimed at protecting xenografts from the adaptive immune response has been made recently. For example, knock-in of CTLA4-Ig or the high-affinity variant LEA29Y (36, 53), knockout or knockdown swine leukocyte antigen (SLA) class I and class II (37, 54), and in vitro tests on SLA class I and class II-silenced cells have reported significantly reduced xenogeneic T cell and natural killer cell responses, and antibody-mediated cell-dependent responses to islet cell clusters (55). However, CTLA4-Ig or LEA29Y transgenic pigs face the problems of hypoimmunity (36, 56).

Immune checkpoint blockade is a promising approach to control pathogenic immune responses. Immunomodulation with PD-L1 improves islet allotransplantation outcomes (57–63), and may facilitate successful xenotransplantation. PD-L1 is a ligand that reduces the proliferation and activation of T cells, B cells, and monocytes through interaction with PD-L1 receptors on these cells, and prevents cell-mediated lysis from CD8⁺ T cells by reducing their proliferation and cytokine secretion (40). Programmed cell death protein 1 blockade has successfully achieved clinical objectives in the treatment of cancer (64–66). In xenotransplantation, pigs transgenic for PD-L1 have been successfully generated, and cells from these pigs prevent human T cell cytotoxicity and B cell activation in vitro (57, 58), with similar results in a pig-to-rat xenotransplantation model (67). In contrast, islet PD-L1 deficiency has been associated with increased allograft rejection and increased inflammatory cell infiltration (68). Testing of the transplantation of pig islets expressing PD-L1 in NHPs should be a future research direction.

In summary, whether the 4th xenoantigen is exposed in islets after CMAHKO remains uncertain, and more research on the cellular response (that will be the next obstacle to explore) is required (69).

Immunosuppressive Regimen

The main objective of the immunosuppressive regimen is to inhibit T cell activation and prevent subsequent T cell-dependent dendritic cell activation and activation of B cells and macrophages. Immunosuppressive regimens based on conventional (FDA-approved) therapy have proved inadequate, although islet graft survival of 222 days has been reported (70). In contrast, blockade of the CD40/CD154 costimulation pathway has resulted in maximal islet graft survival of 965 days (Table 5) (7, 13, 70–76). The major mechanistic effects, advantages, and side-effects of the key immunosuppressive agents of relevance to xenotransplantation have been reviewed by Bikhet and his colleagues (77). Samy et al. have reviewed the role of costimulation pathway blockade in xenotransplantation (78). Here we will focus on novel immunosuppressive regimens based on blockade of the CD40/CD154 costimulation pathway.

Immunosuppressive Regimens Based on Anti-CD40mAbs

Anti-CD40mAbs are a chimeric form of Fab combined with IgG Fc fragments to prevent the stimulation of B and T cells through blockade of the CD40/CD154 pathway, which also participates in regulating thrombosis, tissue inflammation, and hematopoiesis (79). Unlike anti-CD154mAbs, no significant thrombogenic complications have been observed in anti-CD40mAb studies (10). Islet graft survivals are summarized in Table 5.

To date, some anti-CD40mAbs have completed phase II clinical trials of allotransplantation (but not in islet transplantation). These included bleselumab (ASKP1240), iscalimab (CFZ533), and BI 655064 (10, 80, 81). Among them, ASKP1240 demonstrated good results with a favorable benefit-risk ratio and no thromboembolic events in a phase II clinical kidney transplantation trial (10). Treatment with 2C10R4 was associated with the longest pig islet graft survival in NHPs to date (maximum insulin-independence 950 days, maximum graft survival 965 days) (7). However, anti-CD40mAbs may be associated with adverse effects, e.g., a temporary increase in liver enzymes (ASKP1240) (82, 83), significant depletion of peripheral blood B cells (Chi220) (13), and inhibition of T regulatory cell (Treg) expansion (2C10R4) (84).

Immunosuppressive Regimens Based on Anti-CD154 Agents

Anti-CD154 agents also provide efficient CD40/CD154 pathway blockade (85), but were originally associated with thromboembolic complications (BG9588, hu5c8, IDEC-131, ABI793) (86–88), although the situation with IDEC-131 remains controversial (89). They were demonstrated to be preferable to anti-C40mAbs in pig islet transplantation in NHPs (Table 5) (72, 75). Modifications to the Fc region on CD154 agents, the binding site for the Fc receptor (FcgRIIA) on platelets (85), appear to have eliminated thromboembolic events (e.g., CDP7657 and BMS-986004 in rhesus macaques, and MEDI4920 in cynomolgus monkeys) (77). To date, CDP7657, BMS-986004, and MEDI4920 have completed phase I or II clinical trials (not in islet transplantation) without obvious complications (8, 9, 90–92).

Overall, although anti-CD40mAbs have proved successful in pig-to-NHP islet xenotransplantation, the new anti-CD154 agents may prove preferable for clinical trials (Table 6) (9, 10, 75, 80–83, 90, 92–102). Of importance, ongoing studies at the Massachusetts General Hospital indicate that monotherapy with an anti-CD154mAb (with no additional immunosuppressive therapy) prevents rejection of heterotopic heart and life-supporting kidney allografts in monkeys (Robin Pierson and Tatsuo Kawai, personal communications). This regimen, or a modification of it, has not yet been tested in xenograft models

Bikhet et al. published an immunosuppressive regimen that has proved moderately successful in pig solid organ transplantation in NHPs (77), but such a regimen may be too intensive to warrant use in patients with islet xenografts.

The Instant Blood-Mediated Inflammatory Reaction (IBMIR)

After infusion of islets into the portal vein (the preferred site at present), a substantial percentage of islets are lost in the immediate post-transplant period through an inflammatory response termed IBMIR. The loss is significantly greater if the islets are xeno-islets, e.g., pig islets into NHPs and pig islets to human blood in vitro (103–107). Coagulation, platelet aggregation, complement activation, and neutrophil and monocyte infiltration play roles in this reaction (108). Several approaches to reduce the loss of islets have been explored, e.g., anticoagulation, complement depletion (109), and modified islet culture medium (110), but none has been entirely successful yet. The transplantation of islets from pigs with one or multiple genetic modifications may help protect the islets from early injury and loss (14, 74, 111–115). Moreover, alternative transplantation sites in intrapleural space greatly reduced IBMIR (116).

It is beneficial to add heparin or dextran sulfate to the peri-transplant regimen for their anticoagulant and complement-modulating properties that reduce islet loss from IBMIR (109, 117–120). Low molecular dextran sulfate at low doses demonstrated good results in the prevention of IBMIR in phase II clinical islet allotransplantation study (NCT00789308) (119). Nanoparticle-based techniques improve the therapeutic efficacy of heparin. For example, polymeric nanocoating islets with heparin-polyethylene glycol (PEG) or chondroitin sulfate-PEG in an NHP islet allotransplant model was associated with significantly longer islet survival with reduced loss to IBMIR compared with PEG and naked islets (121, 122). Conjugated nanoparticles (heparin-immobilized superparamagnetic iron oxide) conjugated onto the surface of the islets attenuated IBMIR in a rat-to-mouse islet xenotransplantation model (123). Islet-surface modifications with streptavidin-CD47 protein, a chimeric construct expressing CD47 on the extracellular domain, efficiently prevent islet loss from IBMIR (124).

Cibinetide (Araim Pharmaceuticals Inc., Tarrytown, NY, USA) (a non-hematopoietic erythropoietin analogue) also showed islet-protective effects by reducing IBMIR-induced platelet consumption (125). Based on these studies, agents that reduce IBMIR, combined with the transplantation of islets from genetically-engineered pigs (e.g., pigs not expressing the known carbohydrate xenoantigens, but expressing human complement- and coagulation-regulatory proteins), and an optimal immunosuppressive regimen may increase graft survival and the therapeutic efficacy of islet xenotransplantation.

Comment

Key factors in successfully developing pig islet xenotransplantation include determination of the optimal age of the islet-source pig (adult or neonatal), the optimal genetic modifications that should be made to the pig, and the optimal immunosuppressive regimen that should be administered to the recipient. Whether the ‘4th’ xenoantigen is problematic in the pig-to-NHP islet transplantation model needs to be clarified. More attention needs to be directed to genetic modifications that might reduce the instant blood-mediated inflammatory reaction and/or the adaptive immune response to pig islets. The advantages and disadvantages of immunosuppressive regimens based on anti-CD40 and anti-CD154 agents require clarification. Since the first case of successful pig-to-human kidney and heart transplantation had been reported recently (126, 127), we anticipate that pig islet xenotransplantation will become clinically successful when these remaining questions have been resolved.

Funding

This work was supported by grants from the Shenzhen Foundation of Science and Technology (grant numbers GJHZ20200731095207021), the National Key R&D Program of China (2017YFC1103704) and from the Special Funds for the Construction of High Level Hospitals in Guangdong Province (2019).

Publisher’s Note

All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article, or claim that may be made by its manufacturer, is not guaranteed or endorsed by the publisher.

References

• 1

  DiMeglioLAEvans-MolinaCOramRA. Type 1 Diabetes. Lancet (2018) 391:2449–62. doi: 10.1016/S0140-6736(18)31320-5

  • CrossRef
  • Google Scholar

• 2

  LiuZHuWHeTDaiYHaraHBottinoRet al. Pig-to-Primate Islet Xenotransplantation: Past, Present, and Future. Cell Transplant (2017) 26:925–47. doi: 10.3727/096368917X694859

  • CrossRef
  • Google Scholar

• 3

  NagarajuSBottinoRWijkstromMTruccoMCooperDKC. Islet Xenotransplantation: What Is the Optimal Age of the Islet-Source Pig? Xenotransplantation (2015) 22:7–19. doi: 10.1111/xen.12130

  • CrossRef
  • Google Scholar

• 4

  CooperDKCHaraHIwaseHYamamotoTLiQEzzelarabMet al. Justification of Specific Genetic Modifications in Pigs for Clinical Organ Xenotransplantation. Xenotransplantation (2019) 26:e12516. doi: 10.1111/xen.12516

  • CrossRef
  • Google Scholar

• 5

  EstradaJLMartensGLiPAdamsANewellKAFordMLet al. Evaluation of Human and Non-Human Primate Antibody Binding to Pig Cells Lacking GGTA1/CMAH/β4galnt2 Genes. Xenotransplantation (2015) 22:194–202. doi: 10.1111/xen.12161

  • CrossRef
  • Google Scholar

• 6

  HongS-HKimH-JKangS-JParkC-G. Novel Immunomodulatory Approaches for Porcine Islet Xenotransplantation. Curr Diabetes Rep (2021) 21:3. doi: 10.1007/s11892-020-01368-y

  • CrossRef
  • Google Scholar

• 7

  ShinJ-SMinB-HKimJ-MKimJ-SYoonIHKimHJet al. Failure of Transplantation Tolerance Induction by Autologous Regulatory T Cells in the Pig-to-Non-Human Primate Islet Xenotransplantation Model. Xenotransplantation (2016) 23:300–9. doi: 10.1111/xen.12246

  • CrossRef
  • Google Scholar

• 8

  KarnellJLAlbulescuMDrabicSWangLMoateRBacaMet al. A CD40L-Targeting Protein Reduces Autoantibodies and Improves Disease Activity in Patients With Autoimmunity. Sci Transl Med (2019) 11:eaar6584. doi: 10.1126/scitranslmed.aar6584

  • CrossRef
  • Google Scholar

• 9

  ChamberlainCColmanPJRangerAMBurklyLCJohnstonGIOtoulCet al. Repeated Administration of Dapirolizumab Pegol in a Randomised Phase I Study Is Well Tolerated and Accompanied by Improvements in Several Composite Measures of Systemic Lupus Erythematosus Disease Activity and Changes in Whole Blood Transcriptomic Profiles. Ann Rheum Dis (2017) 76:1837–44. doi: 10.1136/annrheumdis-2017-211388

  • CrossRef
  • Google Scholar

• 10

  HarlandRCKlintmalmGJensikSYangHBrombergJHolmanJet al. Efficacy and Safety of Bleselumab in Kidney Transplant Recipients: A Phase 2, Randomized, Open-Label, Noninferiority Study. Am J Transplant (2020) 20:159–71. doi: 10.1111/ajt.15591

  • CrossRef
  • Google Scholar

• 11

  BottinoRBalamuruganANSmetankaCBerteraSHeJRoodPPMet al. Isolation Outcome and Functional Characteristics of Young and Adult Pig Pancreatic Islets for Transplantation Studies. Xenotransplantation (2007) 14:74–82. doi: 10.1111/j.1399-3089.2006.00374.x

  • CrossRef
  • Google Scholar

• 12

  KwakKParkJ-KShimJKoNKimH-JLeeYet al. Comparison of Islet Isolation Result and Clinical Applicability According to GMP-Grade Collagenase Enzyme Blend in Adult Porcine Islet Isolation and Culture. Xenotransplantation (2021) 28:e12703. doi: 10.1111/xen.12703

  • CrossRef
  • Google Scholar

• 13

  ThompsonPCardonaKRussellMBadellIRShafferVKorbuttGet al. CD40-Specific Costimulation Blockade Enhances Neonatal Porcine Islet Survival in Nonhuman Primates. Am J Transplant (2011) 11:947–57. doi: 10.1111/j.1600-6143.2011.03509.x

  • CrossRef
  • Google Scholar

• 14

  ThompsonPBadellIRLoweMCanoJSongMLeopardiFet al. Islet Xenotransplantation Using Gal-Deficient Neonatal Donors Improves Engraftment and Function. Am J Transplant (2011) 11:2593–602. doi: 10.1111/j.1600-6143.2011.03720.x

  • CrossRef
  • Google Scholar

• 15

  ThompsonPBadellIRLoweMTurnerACanoJAvilaJet al. Alternative Immunomodulatory Strategies for Xenotransplantation: CD40/154 Pathway-Sparing Regimens Promote Xenograft Survival. Am J Transplant (2012) 12:1765–75. doi: 10.1111/j.1600-6143.2012.04031.x

  • CrossRef
  • Google Scholar

• 16

  CardonaKKorbuttGSMilasZLyonJCanoJJiangWet al. Long-Term Survival of Neonatal Porcine Islets in Nonhuman Primates by Targeting Costimulation Pathways. Nat Med (2006) 12:304–6. doi: 10.1038/nm1375

  • CrossRef
  • Google Scholar

• 17

  VanderscheldenRSathialingamMAlexanderMLakeyJRT. Cost and Scalability Analysis of Porcine Islet Isolation for Islet Transplantation: Comparison of Juvenile, Neonatal and Adult Pigs. Cell Transplant (2019) 28:967–72. doi: 10.1177/0963689719847460

  • CrossRef
  • Google Scholar

• 18

  LauHCorralesNRodriguezSLuongCZaldivarFAlexanderMet al. An Islet Maturation Media to Improve the Development of Young Porcine Islets During In Vitro Culture. Islets (2020) 12:41–58. doi: 10.1080/19382014.2020.1750933

  • CrossRef
  • Google Scholar

• 19

  HeSWangCDuXChenYZhaoJTianBet al. MSCs Promote the Development and Improve the Function of Neonatal Porcine Islet Grafts. FASEB J (2018) 32:3242–53. doi: 10.1096/fj.201700991R

  • CrossRef
  • Google Scholar

• 20

  MontanariESzabóLBalaphasAMeyerJPerriraz-MayerNPimentaJet al. Multipotent Mesenchymal Stromal Cells Derived From Porcine Exocrine Pancreas Improve Insulin Secretion From Juvenile Porcine Islet Cell Clusters. Xenotransplantation (2021) 28:e12666. doi: 10.1111/xen.12666

  • CrossRef
  • Google Scholar

• 21

  HassounaTSeebergerKLSalamaBKorbuttGS. Functional Maturation and In Vitro Differentiation of Neonatal Porcine Islet Grafts. Transplantation (2018) 102:e413–23. doi: 10.1097/TP.0000000000002354

  • CrossRef
  • Google Scholar

• 22

  SmithKEPurvisWGDavisMAMinCGCookseyAMWeberCSet al. In Vitro Characterization of Neonatal, Juvenile, and Adult Porcine Islet Oxygen Demand, β-Cell Function, and Transcriptomes. Xenotransplantation (2018) 25:e12432. doi: 10.1111/xen.12432

  • CrossRef
  • Google Scholar

• 23

  EmamaulleeJAShapiroAMJRajotteRVKorbuttGElliottJF. Neonatal Porcine Islets Exhibit Natural Resistance to Hypoxia-Induced Apoptosis. Transplantation (2006) 82:945–52. doi: 10.1097/01.tp.0000238677.00750.32

  • CrossRef
  • Google Scholar

• 24

  DaiYVaughtTDBooneJChenS-HPhelpsCJBallSet al. Targeted Disruption of the Alpha1,3-Galactosyltransferase Gene in Cloned Pigs. Nat Biotechnol (2002) 20:251–5. doi: 10.1038/nbt0302-251

  • CrossRef
  • Google Scholar

• 25

  PhelpsCJKoikeCVaughtTDBooneJWellsKDChenS-Het al. Production of Alpha 1,3-Galactosyltransferase-Deficient Pigs. Science (2003) 299:411–4. doi: 10.1126/science.1078942

  • CrossRef
  • Google Scholar

• 26

  KimGALeeEMJinJ-XLeeSTaweechaipaisankulAHwangJIet al. Generation of CMAHKO/GTKO/shTNFRI-Fc/HO-1 Quadruple Gene Modified Pigs. Transgenic Res (2017) 26:435–45. doi: 10.1007/s11248-017-0021-6

  • CrossRef
  • Google Scholar

• 27

  WangR-GRuanMZhangR-JChenLLiX-XFangBet al. Antigenicity of Tissues and Organs From GGTA1/CMAH/β4galnt2 Triple Gene Knockout Pigs. J BioMed Res (2018) 33:194–202. doi: 10.7555/JBR.32.20180018

  • CrossRef
  • Google Scholar

• 28

  KimGALeeEMChoBAlamZKimSJLeeSet al. Generation by Somatic Cell Nuclear Transfer of GGTA1 Knockout Pigs Expressing Soluble Human TNFRI-Fc and Human HO-1. Transgenic Res (2019) 28:91–102. doi: 10.1007/s11248-018-0103-0

  • CrossRef
  • Google Scholar

• 29

  DiamondLEQuinnCMMartinMJLawsonJPlattJLLoganJS. A Human CD46 Transgenic Pig Model System for the Study of Discordant Xenotransplantation. Transplantation (2001) 71:132–42. doi: 10.1097/00007890-200101150-00021

  • CrossRef
  • Google Scholar

• 30

  MurakamiHNagashimaHTakahagiYFujimuraTMiyagawaSOkabeMet al. Production of Transgenic Pigs Expressing Human DAF (CD55) Regulated by the Porcine MCP Gene Promoter. Transplant Proc (2000) 32:2505–6. doi: 10.1016/s0041-1345(00)01769-3

  • CrossRef
  • Google Scholar

• 31

  NiemannHVerhoeyenEWonigeitKLorenzRHeckerJSchwinzerRet al. Cytomegalovirus Early Promoter Induced Expression of Hcd59 in Porcine Organs Provides Protection Against Hyperacute Rejection. Transplantation (2001) 72:1898–906. doi: 10.1097/00007890-200112270-00006

  • CrossRef
  • Google Scholar

• 32

  PetersenBRamackersWTiedeALucas-HahnAHerrmannDBarg-KuesBet al. Pigs Transgenic for Human Thrombomodulin Have Elevated Production of Activated Protein C. Xenotransplantation (2009) 16:486–95. doi: 10.1111/j.1399-3089.2009.00537.x

  • CrossRef
  • Google Scholar

• 33

  ChoJKimGQamarAYFangXRoyPKTangaBMet al. Improved Efficiencies in the Generation of Multigene-Modified Pigs by Recloning and Using Sows as the Recipient. Zygote (2021) 30:1–8. doi: 10.1017/S0967199421000423

  • CrossRef
  • Google Scholar

• 34

  AhrensHPetersenBCunhaAQueisserA-LHerrmannDKuesWet al. Production and Characterization of TF Knock-Down Pigs and hTFPI Transgenic Pigs. Xenotransplantation (2011) 18:296–6. doi: 10.1111/j.1399-3089.2011.00661.x

  • CrossRef
  • Google Scholar

• 35

  ChoiKShimJKoNEomHKimJLeeJ-Wet al. Production of Heterozygous Alpha 1,3-Galactosyltransferase (GGTA1) Knock-Out Transgenic Miniature Pigs Expressing Human CD39. Transgenic Res (2017) 26:209–24. doi: 10.1007/s11248-016-9996-7

  • CrossRef
  • Google Scholar

• 36

  BährAKäserTKemterEGernerWKuromeMBaarsWet al. Ubiquitous Lea29y Expression Blocks T Cell Co-Stimulation But Permits Sexual Reproduction in Genetically Modified Pigs. PloS One (2016) 11:e0155676. doi: 10.1371/journal.pone.0155676

  • CrossRef
  • Google Scholar

• 37

  HaraHWittWCrossleyTLongCIsseKFanLet al. Human Dominant-Negative Class II Transactivator Transgenic Pigs - Effect on the Human Anti-Pig T-Cell Immune Response and Immune Status. Immunology (2013) 140:39–46. doi: 10.1111/imm.12107

  • CrossRef
  • Google Scholar

• 38

  WangYDuYZhouXWangLLiJWangFet al. Efficient Generation of B2m-Null Pigs via Injection of Zygote With TALENs. Sci Rep (2016) 6:38854. doi: 10.1038/srep38854

  • CrossRef
  • Google Scholar

• 39

  TenaAGermanaSTurcotteNLeto BaroneAAArnSTerlouwSLet al. Miniature Swine Expressing Human Cd47 to Enhance Bone Marrow Engraftment in Non-Human Primates: 1651. Transplantation (2012) 94:776. doi: 10.1097/00007890-201211271-01520

  • CrossRef
  • Google Scholar

• 40

  BuermannAPetkovSPetersenBHeinRLucas-HahnABaarsWet al. Pigs Expressing the Human Inhibitory Ligand PD-L1 (CD 274) Provide a New Source of Xenogeneic Cells and Tissues With Low Immunogenic Properties. Xenotransplantation (2018) 25:e12387. doi: 10.1111/xen.12387

  • CrossRef
  • Google Scholar

• 41

  YueYXuWKanYZhaoH-YZhouYSongXet al. Extensive Germline Genome Engineering in Pigs. Nat BioMed Eng (2021) 5:134–43. doi: 10.1038/s41551-020-00613-9

  • CrossRef
  • Google Scholar

• 42

  FooteJBJagdaleAYamamotoTHaraHBikhetMHSchuurmanH-Jet al. Histopathology of Pig Kidney Grafts With/Without Expression of the Carbohydrate Neu5Gc in Immunosuppressed Baboons. Xenotransplantation (2021) 28:e12715. doi: 10.1111/xen.12715

  • CrossRef
  • Google Scholar

• 43

  AriyoshiYTakeuchiKPomposelliTEkanayake-AlperDKShimizuABoydLet al. Antibody Reactivity With New Antigens Revealed in Multi-Transgenic Triple Knockout Pigs may Cause Early Loss of Pig Kidneys in Baboons. Xenotransplantation (2021) 28:e12642. doi: 10.1111/xen.12642

  • CrossRef
  • Google Scholar

• 44

  YamamotoTHaraHIwaseHJagdaleABikhetMHMorsiMAet al. The Final Obstacle to Successful Pre-Clinical Xenotransplantation? Xenotransplantation (2020) 27:e12596. doi: 10.1111/xen.12596

  • CrossRef
  • Google Scholar

• 45

  YamamotoTIwaseHPatelDJagdaleAAyaresDAndersonDet al. Old World Monkeys Are Less Than Ideal Transplantation Models for Testing Pig Organs Lacking Three Carbohydrate Antigens (Triple-Knockout). Sci Rep (2020) 10:9771. doi: 10.1038/s41598-020-66311-3

  • CrossRef
  • Google Scholar

• 46

  YamamotoTHaraHAyaresDCooperDKC. The Problem of the “4th Xenoantigen” After Pig Organ Transplantation in Non-Human Primates may be Overcome by Expression of Human “Protective” Proteins. Xenotransplantation (2021) 28:e12658. doi: 10.1111/xen.12658

  • CrossRef
  • Google Scholar

• 47

  LeeWHaraHEzzelarabMBIwaseHBottinoRLongCet al. Initial In Vitro Studies on Tissues and Cells From GTKO/CD46/NeuGcKO Pigs. Xenotransplantation (2016) 23:137–50. doi: 10.1111/xen.12229

  • CrossRef
  • Google Scholar

• 48

  ChoeHMLuoZ-BKangJ-DOhMJAnHJYinX-J. Pathological Features in “Humanized” Neonatal Pig. Anim Biotechnol (2021), 1–9. doi: 10.1080/10495398.2021.1962896

  • CrossRef
  • Google Scholar

• 49

  ObukhovaPTsygankovaSChinarevAShilovaNNokelAKosmaPet al. Are There Specific Antibodies Against Neu5Gc Epitopes in the Blood of Healthy Individuals? Glycobiology (2020) 30:395–406. doi: 10.1093/glycob/cwz107

  • CrossRef
  • Google Scholar

• 50

  NannoYShajahanASononRNAzadiPHeringBJBurlakC. High-Mannose Type N-Glycans With Core Fucosylation and Complex-Type N-Glycans With Terminal Neuraminic Acid Residues Are Unique to Porcine Islets. PloS One (2020) 15:e0241249. doi: 10.1371/journal.pone.0241249

  • CrossRef
  • Google Scholar

• 51

  NannoYSternerEGildersleeveJCHeringBJBurlakC. Carbohydrate Antigen Microarray Analysis of Serum IgG and IgM Antibodies Before and After Adult Porcine Islet Xenotransplantation in Cynomolgus Macaques. PloS One (2021) 16:e0253029. doi: 10.1371/journal.pone.0253029

  • CrossRef
  • Google Scholar

• 52

  NannoYSternerEGildersleeveJCHeringBJBurlakC. Profiling Natural Serum Antibodies of Non-Human Primates With a Carbohydrate Antigen Microarray. Xenotransplantation (2020) 27:e12567. doi: 10.1111/xen.12567

  • CrossRef
  • Google Scholar

• 53

  BuerckLWSchusterMOduncuFSBaehrAMayrTGuethoffSet al. LEA29Y Expression in Transgenic Neonatal Porcine Islet-Like Cluster Promotes Long-Lasting Xenograft Survival in Humanized Mice Without Immunosuppressive Therapy. Sci Rep (2017) 7:3572. doi: 10.1038/s41598-017-03913-4

  • CrossRef
  • Google Scholar

• 54

  FischerKRieblingerBHeinRSfrisoRZuberJFischerAet al. Viable Pigs After Simultaneous Inactivation of Porcine MHC Class I and Three Xenoreactive Antigen Genes GGTA1, CMAH and B4GALNT2. Xenotransplantation (2020) 27:e12560. doi: 10.1111/xen.12560

  • CrossRef
  • Google Scholar

• 55

  Carvalho OliveiraMValdiviaEVerboomMYuzefovychYSakeHJPogozhykhOet al. Generating Low Immunogenic Pig Pancreatic Islet Cell Clusters for Xenotransplantation. J Cell Mol Med (2020) 24:5070–81. doi: 10.1111/jcmm.15136

  • CrossRef
  • Google Scholar

• 56

  PhelpsCJBallSFVaughtTDVanceAMMendicinoMMonahanJAet al. Production and Characterization of Transgenic Pigs Expressing Porcine CTLA4-Ig. Xenotransplantation (2009) 16:477–85. doi: 10.1111/j.1399-3089.2009.00533.x

  • CrossRef
  • Google Scholar

• 57

  DingQLuLZhouXZhouYChouK-Y. Human PD-L1-Overexpressing Porcine Vascular Endothelial Cells Induce Functionally Suppressive Human CD4+CD25hiFoxp3+ Treg Cells. J Leukoc Biol (2011) 90:77–86. doi: 10.1189/jlb.1210691

  • CrossRef
  • Google Scholar

• 58

  BuermannARömermannDBaarsWHundrieserJKlempnauerJSchwinzerR. Inhibition of B-Cell Activation and Antibody Production by Triggering Inhibitory Signals via the PD-1/PD-Ligand Pathway. Xenotransplantation (2016) 23:347–56. doi: 10.1111/xen.12261

  • CrossRef
  • Google Scholar

• 59

  LiRLeeJKimMLiuVMoulikMLiHet al. PD-L1-Driven Tolerance Protects Neurogenin3-Induced Islet Neogenesis to Reverse Established Type 1 Diabetes in NOD Mice. Diabetes (2015) 64:529–40. doi: 10.2337/db13-1737

  • CrossRef
  • Google Scholar

• 60

  BatraLShresthaPZhaoHWoodwardKBTogayATanMet al. Localized Immunomodulation With PD-L1 Results in Sustained Survival and Function of Allogeneic Islets Without Chronic Immunosuppression. J Immunol (2020) 204:2840–51. doi: 10.4049/jimmunol.2000055

  • CrossRef
  • Google Scholar

• 61

  CoronelMMMartinKEHuncklerMDBarberGO’NeillEBMedinaJDet al. Immunotherapy via PD-L1-Presenting Biomaterials Leads to Long-Term Islet Graft Survival. Sci Adv (2020) 6:eaba5573. doi: 10.1126/sciadv.aba5573

  • CrossRef
  • Google Scholar

• 62

  LiTMaRZhuJYWangFSHuangLLengXS. PD-1/PD-L1 Costimulatory Pathway-Induced Mouse Islet Transplantation Immune Tolerance. Transplant Proc (2015) 47:165–70. doi: 10.1016/j.transproceed.2014.10.043

  • CrossRef
  • Google Scholar

• 63

  LiTMaRZhuJWangFHuangLLengX. Blockade of the OX40/OX40L Pathway and Induction of PD-L1 Synergistically Protects Mouse Islet Allografts From Rejection. Chin Med J (Engl) (2014) 127:2686–92. doi: 10.3760/cma.j.issn.0366-6999.20140740

  • CrossRef
  • Google Scholar

• 64

  KraehenbuehlLWengC-HEghbaliSWolchokJDMerghoubT. Enhancing Immunotherapy in Cancer by Targeting Emerging Immunomodulatory Pathways. Nat Rev Clin Oncol (2022) 19:37–50. doi: 10.1038/s41571-021-00552-7

  • CrossRef
  • Google Scholar

• 65

  LemaireVShemeshCSRotteA. Pharmacology-Based Ranking of Anti-Cancer Drugs to Guide Clinical Development of Cancer Immunotherapy Combinations. J Exp Clin Cancer Res (2021) 40:311. doi: 10.1186/s13046-021-02111-5

  • CrossRef
  • Google Scholar

• 66

  TanACBagleySJWenPYLimMPlattenMColmanHet al. Systematic Review of Combinations of Targeted or Immunotherapy in Advanced Solid Tumors. J Immunother Cancer (2021) 9:e002459. doi: 10.1136/jitc-2021-002459

  • CrossRef
  • Google Scholar

• 67

  Plege-FleckALiekeTRömermannDDüvelHHundrieserJBuermannAet al. Pig to Rat Cell Transplantation: Reduced Cellular and Antibody Responses to Xenografts Overexpressing PD-L1. Xenotransplantation (2014) 21:533–42. doi: 10.1111/xen.12121

  • CrossRef
  • Google Scholar

• 68

  MaDDuanWLiYWangZLiSGongNet al. PD-L1 Deficiency Within Islets Reduces Allograft Survival in Mice. PloS One (2016) 11:e0152087. doi: 10.1371/journal.pone.0152087

  • CrossRef
  • Google Scholar

• 69

  LadowskiJMartensGEstradaJTectorMTectorJ. The Desirable Donor Pig to Eliminate All Xenoreactive Antigens. Xenotransplantation (2019) 26:e12504. doi: 10.1111/xen.12504

  • CrossRef
  • Google Scholar

• 70

  KimJ-MHongS-HChungHShinJ-SMinB-HKimHJet al. Long-Term Porcine Islet Graft Survival in Diabetic Non-Human Primates Treated With Clinically Available Immunosuppressants. Xenotransplantation (2021) 28:e12659. doi: 10.1111/xen.12659

  • CrossRef
  • Google Scholar

• 71

  LeeJ-IKimJChoiY-JParkH-JParkH-JWiHJet al. The Effect of Epitope-Based Ligation of ICAM-1 on Survival and Retransplantation of Pig Islets in Nonhuman Primates. Xenotransplantation (2018) 25:e12362. doi: 10.1111/xen.12362

  • CrossRef
  • Google Scholar

• 72

  ShinJSKimJMKimJSMinBHKimYHKimHJet al. Long-Term Control of Diabetes in Immunosuppressed Nonhuman Primates (NHP) by the Transplantation of Adult Porcine Islets. Am J Transplant (2015) 15:2837–50. doi: 10.1111/ajt.13345

  • CrossRef
  • Google Scholar

• 73

  BottinoRKnollMFGraeme-WilsonJKleinECAyaresDTruccoMet al. Safe Use of Anti-CD154 Monoclonal Antibody in Pig Islet Xenotransplantation in Monkeys. Xenotransplantation (2017) 24:e12283. doi: 10.1111/xen.12283

  • CrossRef
  • Google Scholar

• 74

  van der WindtDJBottinoRCasuACampanileNSmetankaCHeJet al. Long-Term Controlled Normoglycemia in Diabetic Non-Human Primates After Transplantation With Hcd46 Transgenic Porcine Islets. Am J Transplant (2009) 9:2716–26. doi: 10.1111/j.1600-6143.2009.02850.x

  • CrossRef
  • Google Scholar

• 75

  ShinJ-SKimJ-MMinB-HYoonIHKimHJKimJ-Set al. Pre-Clinical Results in Pig-to-Non-Human Primate Islet Xenotransplantation Using Anti-CD40 Antibody (2C10R4)-Based Immunosuppression. Xenotransplantation (2018) 25:e12356. doi: 10.1111/xen.12356

  • CrossRef
  • Google Scholar

• 76

  KimJ-MHongS-HShinJ-SMinB-HKimHJChungHet al. Long-Term Control of Diabetes in a Nonhuman Primate by Two Separate Transplantations of Porcine Adult Islets Under Immunosuppression. Am J Transplant (2021) 21:3561–72. doi: 10.1111/ajt.16704

  • CrossRef
  • Google Scholar

• 77

  BikhetMIwaseHYamamotoTJagdaleAFooteJBEzzelarabMet al. What Therapeutic Regimen Will be Optimal for Initial Clinical Trials of Pig Organ Transplantation? Transplantation (2021) 105:1143–55. doi: 10.1097/TP.0000000000003622

  • CrossRef
  • Google Scholar

• 78

  SamyKPButlerJRLiPCooperDKCEkserB. The Role of Costimulation Blockade in Solid Organ and Islet Xenotransplantation. J Immunol Res (2017) 2017:8415205. doi: 10.1155/2017/8415205

  • CrossRef
  • Google Scholar

• 79

  TangTChengXTruongBSunLYangXWangH. Molecular Basis and Therapeutic Implications of CD40/CD40L Immune Checkpoint. Pharmacol Ther (2021) 219:107709. doi: 10.1016/j.pharmthera.2020.107709

  • CrossRef
  • Google Scholar

• 80

  KahalyGJStanMNFrommerLGergelyPColinLAmerAet al. A Novel Anti-CD40 Monoclonal Antibody, Iscalimab, for Control of Graves Hyperthyroidism-a Proof-of-Concept Trial. J Clin Endocrinol Metab (2020) 105:dgz013. doi: 10.1210/clinem/dgz013

  • CrossRef
  • Google Scholar

• 81

  VisvanathanSDanilukSPtaszyńskiRMüller-LadnerURamanujamMRosenstockBet al. Effects of BI 655064, an Antagonistic Anti-CD40 Antibody, on Clinical and Biomarker Variables in Patients With Active Rheumatoid Arthritis: A Randomised, Double-Blind, Placebo-Controlled, Phase IIa Study. Ann Rheum Dis (2019) 78:754–60. doi: 10.1136/annrheumdis-2018-214729

  • CrossRef
  • Google Scholar

• 82

  VincentiFKlintmalmGYangHRam PeddiVBlahunkaPConkleAet al. A Randomized, Phase 1b Study of the Pharmacokinetics, Pharmacodynamics, Safety, and Tolerability of Bleselumab, a Fully Human, Anti-CD40 Monoclonal Antibody, in Kidney Transplantation. Am J Transplant (2020) 20:172–80. doi: 10.1111/ajt.15560

  • CrossRef
  • Google Scholar

• 83

  Anil KumarMSPappKTainakaRValluriUWangXZhuTet al. Randomized, Controlled Study of Bleselumab (ASKP1240) Pharmacokinetics and Safety in Patients With Moderate-to-Severe Plaque Psoriasis. Biopharm Drug Dispos (2018) 39:245–55. doi: 10.1002/bdd.2130

  • CrossRef
  • Google Scholar

• 84

  OuraTHottaKRosalesIDehnadiAKawaiKLeeHet al. Addition of Anti-CD40 Monoclonal Antibody to Nonmyeloablative Conditioning With Belatacept Abrogated Allograft Tolerance Despite Induction of Mixed Chimerism. Transplantation (2019) 103:168–76. doi: 10.1097/TP.0000000000002417

  • CrossRef
  • Google Scholar

• 85

  LeeJ-IChoiY-JParkH-JJungKCParkSH. RD-05, a Novel Anti-CD154 Antibody, Efficiently Inhibits Generation of Anti-Drug Antibody Without the Risk of Thrombus Formation in Non-Human Primates. Biochem Biophys Res Commun (2018) 498:996–1001. doi: 10.1016/j.bbrc.2018.03.099

  • CrossRef
  • Google Scholar

• 86

  BoumpasDTFurieRManziSIlleiGGWallaceDJBalowJEet al. A Short Course of BG9588 (Anti-CD40 Ligand Antibody) Improves Serologic Activity and Decreases Hematuria in Patients With Proliferative Lupus Glomerulonephritis. Arthritis Rheum (2003) 48:719–27. doi: 10.1002/art.10856

  • CrossRef
  • Google Scholar

• 87

  FerrantJLBenjaminCDCutlerAHKalledSLHsuY-MGarberEAet al. The Contribution of Fc Effector Mechanisms in the Efficacy of Anti-CD154 Immunotherapy Depends on the Nature of the Immune Challenge. Int Immunol (2004) 16:1583–94. doi: 10.1093/intimm/dxh162

  • CrossRef
  • Google Scholar

• 88

  Sifuentes GiraldoWAGarcía VillanuevaMJBoteanuALLois IglesiasAZea MendozaAC. New Targets in Systemic Lupus (Part 2/2). Reumatol Clin (2012) 8:263–9. doi: 10.1016/j.reuma.2012.01.013

  • CrossRef
  • Google Scholar

• 89

  FadulCEMao-DraayerYRyanKANoelleRJWishartHAChannonJYet al. Safety and Immune Effects of Blocking Cd40 Ligand in Multiple Sclerosis. Neurol Neuroimmunol Neuroinflamm (2021) 8:e1096. doi: 10.1212/NXI.0000000000001096

  • CrossRef
  • Google Scholar

• 90

  TocoianABuchanPKirbyHSoransonJZamaconaMWalleyRet al. First-In-Human Trial of the Safety, Pharmacokinetics and Immunogenicity of a PEGylated Anti-CD40L Antibody Fragment (CDP7657) in Healthy Individuals and Patients With Systemic Lupus Erythematosus. Lupus (2015) 24:1045–56. doi: 10.1177/0961203315574558

  • CrossRef
  • Google Scholar

• 91

  KimSCWakweWHigginbothamLBMathewsDVBreedenCPStephensonACet al. Fc-Silent Anti-Cd154 Domain Antibody Effectively Prevents Nonhuman Primate Renal Allograft Rejection. Am J Transplant (2017) 17:1182–92. doi: 10.1111/ajt.14197

  • CrossRef
  • Google Scholar

• 92

  FurieRABruceINDörnerTLeonMGLeszczyńskiPUrowitzMet al. Phase 2, Randomized, Placebo-Controlled Trial of Dapirolizumab Pegol in Patients With Moderate-to-Severe Active Systemic Lupus Erythematosus. Rheumatol (Oxford) (2021) 60:keab381. doi: 10.1093/rheumatology/keab381

  • CrossRef
  • Google Scholar

• 93

  GoldwaterRKeirnsJBlahunkaPFirstRSawamotoTZhangWet al. A Phase 1, Randomized Ascending Single-Dose Study of Antagonist Anti-Human CD40 ASKP1240 in Healthy Subjects. Am J Transplant (2013) 13:1040–6. doi: 10.1111/ajt.12082

  • CrossRef
  • Google Scholar

• 94

  EspiéPHeYKooPSickertDDupuyCChokotéEet al. First-In-Human Clinical Trial to Assess Pharmacokinetics, Pharmacodynamics, Safety, and Tolerability of Iscalimab, an Anti-CD40 Monoclonal Antibody. Am J Transplant (2020) 20:463–73. doi: 10.1111/ajt.15661

  • CrossRef
  • Google Scholar

• 95

  CNI-Free Therapy With Iscalimab (Anti-Cd40 Mab) Preserves Allograft Histology Compared to Standard of Care After Kidney Transplantation, in: ATC Abstracts. Available at: https://atcmeetingabstracts.com/abstract/cni-free-therapy-with-iscalimab-anti-cd40-mab-preserves-allograft-histology-compared-to-standard-of-care-after-kidney-transplantation/ (Accessed December 17, 2021).

  • Google Scholar

• 96

  CFZ533, A New Anti-Cd40 Mab Demonstrates Comparable Efficacy and Better Renal Function Versus Tacrolimus in De-Novo Cni-Free Kidney Transplantation, in: ATC Abstracts. Available at: https://atcmeetingabstracts.com/abstract/cfz533-a-new-anti-cd40-mab-demonstrates-comparable-efficacy-and-better-renal-function-versus-tacrolimus-in-de-novo-cni-free-kidney-transplantation/ (Accessed December 17, 2021).

  • Google Scholar

• 97

  FisherBASzantoANgW-FBombardieriMPoschMGPapasASet al. Assessment of the Anti-CD40 Antibody Iscalimab in Patients With Primary Sjögren’s Syndrome: A Multicentre, Randomised, Double-Blind, Placebo-Controlled, Proof-of-Concept Study. Lancet Rheumatol (2020) 2:e142–52. doi: 10.1016/S2665-9913(19)30135-3

  • CrossRef
  • Google Scholar

• 98

  SchwabeCRosenstockBDoanTHamiltonPDunbarPREleftherakiAGet al. Safety, Pharmacokinetics, and Pharmacodynamics of Multiple Rising Doses of Bi 655064, an Antagonistic Anti-CD40 Antibody, in Healthy Subjects: A Potential Novel Treatment for Autoimmune Diseases. J Clin Pharmacol (2018) 58:1566–77. doi: 10.1002/jcph.1278

  • CrossRef
  • Google Scholar

• 99

  JayneDSteffgenJRomero-DiazJAmanoHNoppakunKGomezHMet al. Pos0687 a Randomised Dose Ranging, Placebo-Controlled, Phase Ii Study Assessing the Efficacy and Safety of Bi 655064, an Antagonistic Anti-CD40 Antibody, in Patients With Lupus Nephritis. Ann Rheumatic Dis (2021) 80:589–90. doi: 10.1136/annrheumdis-2021-eular.1401

  • CrossRef
  • Google Scholar

• 100

  Kiniksa Announces Positive Final Data From Phase 1 Trial of KPL-404, in: Kiniksa Pharmaceuticals. Available at: https://investors.kiniksa.com/news-releases/news-release-details/kiniksa-announces-positive-final-data-phase-1-trial-kpl-404/ (Accessed October 29, 2021).

  • Google Scholar

• 101

  MohiuddinMMSinghAKCorcoranPCThomas IiiMLClarkTLewisBGet al. Chimeric 2C10R4 Anti-CD40 Antibody Therapy Is Critical for Long-Term Survival of GTKO.hCD46.hTBM Pig-to-Primate Cardiac Xenograft. Nat Commun (2016) 7:11138. doi: 10.1038/ncomms11138

  • CrossRef
  • Google Scholar

• 102

  SinghARamachandranSGrahamMLDaneshmandiSHellerDSuarez-PinzonWLet al. Long-Term Tolerance of Islet Allografts in Nonhuman Primates Induced by Apoptotic Donor Leukocytes. Nat Commun (2019) 10:3495. doi: 10.1038/s41467-019-11338-y

  • CrossRef
  • Google Scholar

• 103

  KimJHOhBJLeeHNParkHSParkSGParkKS. Endothelial Colony-Forming Cell Coating of Pig Islets Prevents Xenogeneic Instant Blood-Mediated Inflammatory Reaction. Cell Transplant (2011) 20:1805–15. doi: 10.3727/096368911X566154

  • CrossRef
  • Google Scholar

• 104

  van der WindtDJBottinoRCasuACampanileNCooperDKC. Rapid Loss of Intraportally Transplanted Islets: An Overview of Pathophysiology and Preventive Strategies. Xenotransplantation (2007) 14:288–97. doi: 10.1111/j.1399-3089.2007.00419.x

  • CrossRef
  • Google Scholar

• 105

  NagarajuSBerteraSTanakaTHaraHRayatGRWijkstromMet al. In Vitro Exposure of Pig Neonatal Isletlike Cell Clusters to Human Blood. Xenotransplantation (2015) 22:317–24. doi: 10.1111/xen.12178

  • CrossRef
  • Google Scholar

• 106

  SamyKPDavisRPGaoQMartinBMSongMCanoJet al. Early Barriers to Neonatal Porcine Islet Engraftment in a Dual Transplant Model. Am J Transplant (2018) 18:998–1006. doi: 10.1111/ajt.14601

  • CrossRef
  • Google Scholar

• 107

  van der WindtDJMariglianoMHeJVotyakovaTVEcheverriGJEkserBet al. Early Islet Damage After Direct Exposure of Pig Islets to Blood: Has Humoral Immunity Been Underestimated? Cell Transplant (2012) 21:1791–802. doi: 10.3727/096368912X653011

  • CrossRef
  • Google Scholar

• 108

  MartinBMSamyKPLoweMCThompsonPWCanoJFarrisABet al. Dual Islet Transplantation Modeling of the Instant Blood-Mediated Inflammatory Reaction. Am J Transplant (2015) 15:1241–52. doi: 10.1111/ajt.13098

  • CrossRef
  • Google Scholar

• 109

  RoodPPMBottinoRBalamuruganANSmetankaCAyaresDGrothC-Get al. Reduction of Early Graft Loss After Intraportal Porcine Islet Transplantation in Monkeys. Transplantation (2007) 83:202–10. doi: 10.1097/01.tp.0000250680.36942.c6

  • CrossRef
  • Google Scholar

• 110

  MaXYangCZhangJWangJLiWXuCet al. Culturing With Modified EGM2 Medium Enhances Porcine Neonatal Islet-Like Cell Clusters Resistance to Apoptosis in Islet Xenotransplantation. Xenotransplantation (2018) 25:e12358. doi: 10.1111/xen.12358

  • CrossRef
  • Google Scholar

• 111

  CasuAEcheverriGJBottinoRvan der WindtDJHeJEkserBet al. Insulin Secretion and Glucose Metabolism in Alpha 1,3-Galactosyltransferase Knock-Out Pigs Compared to Wild-Type Pigs. Xenotransplantation (2010) 17:131–9. doi: 10.1111/j.1399-3089.2010.00572.x

  • CrossRef
  • Google Scholar

• 112

  BottinoRWijkstromMvan der WindtDJHaraHEzzelarabMMuraseNet al. Pig-To-Monkey Islet Xenotransplantation Using Multi-Transgenic Pigs. Am J Transplant (2014) 14:2275–87. doi: 10.1111/ajt.12868

  • CrossRef
  • Google Scholar

• 113

  WijkstromMBottinoRIwaseHHaraHEkserBvan der WindtDet al. Glucose Metabolism in Pigs Expressing Human Genes Under an Insulin Promoter. Xenotransplantation (2015) 22:70–9. doi: 10.1111/xen.12145

  • CrossRef
  • Google Scholar

• 114

  SamyKPGaoQDavisRPSongMFitchZWMulvihillMSet al. The Role of Human CD46 in Early Xenoislet Engraftment in a Dual Transplant Model. Xenotransplantation (2019) 26:e12540. doi: 10.1111/xen.12540

  • CrossRef
  • Google Scholar

• 115

  SongMFitchZWSamyKPMartinBMGaoQPatrick DavisRet al. Coagulation, Inflammation, and CD46 Transgene Expression in Neonatal Porcine Islet Xenotransplantation. Xenotransplantation (2021) 28:e12680. doi: 10.1111/xen.12680

  • CrossRef
  • Google Scholar

• 116

  LeiJZhangADengHYangZPetersCWLeeKMet al. Intrapleural Transplantation of Allogeneic Pancreatic Islets Achieves Glycemic Control in a Diabetic Non-Human Primate. Am J Transplant (2021) 22:966–72. doi: 10.1111/ajt.16875

  • CrossRef
  • Google Scholar

• 117

  GustafsonEAsifSKozarcaninHElgueGMeurlingSEkdahlKNet al. Control of Ibmir Induced by Fresh and Cryopreserved Hepatocytes by Low Molecular Weight Dextran Sulfate Versus Heparin. Cell Transplant (2017) 26:71–81. doi: 10.3727/096368916X692609

  • CrossRef
  • Google Scholar

• 118

  JohanssonHGotoMDufraneDSiegbahnAElgueGGianelloPet al. Low Molecular Weight Dextran Sulfate: A Strong Candidate Drug to Block IBMIR in Clinical Islet Transplantation. Am J Transplant (2006) 6:305–12. doi: 10.1111/j.1600-6143.2005.01186.x

  • CrossRef
  • Google Scholar

• 119

  von Zur-MühlenBLundgrenTBaymanLBerneCBridgesNEggermanTet al. Open Randomized Multicenter Study to Evaluate Safety and Efficacy of Low Molecular Weight Sulfated Dextran in Islet Transplantation. Transplantation (2019) 103:630–7. doi: 10.1097/TP.0000000000002425

  • CrossRef
  • Google Scholar

• 120

  CabricSSanchezJLundgrenTFossAFelldinMKällenRet al. Islet Surface Heparinization Prevents the Instant Blood-Mediated Inflammatory Reaction in Islet Transplantation. Diabetes (2007) 56:2008–15. doi: 10.2337/db07-0358

  • CrossRef
  • Google Scholar

• 121

  ParkHHaqueMRParkJBLeeKWLeeSKwonYet al. Polymeric Nano-Shielded Islets With Heparin-Polyethylene Glycol in a Non-Human Primate Model. Biomaterials (2018) 171:164–77. doi: 10.1016/j.biomaterials.2018.04.028

  • CrossRef
  • Google Scholar

• 122

  YangJJiangSGuanYDengJLouSFengDet al. Pancreatic Islet Surface Engineering With a starPEG-Chondroitin Sulfate Nanocoating. Biomater Sci (2019) 7:2308–16. doi: 10.1039/c9bm00061e

  • CrossRef
  • Google Scholar

• 123

  HwangYHKimMJLeeDY. MRI-Sensitive Contrast Agent With Anticoagulant Activity for Surface Camouflage of Transplanted Pancreatic Islets. Biomaterials (2017) 138:121–30. doi: 10.1016/j.biomaterials.2017.05.038

  • CrossRef
  • Google Scholar

• 124

  ShresthaPBatraLTariq MalikMTanMYolcuESShirwanH. Immune Checkpoint CD47 Molecule Engineered Islets Mitigate Instant Blood-Mediated Inflammatory Reaction and Show Improved Engraftment Following Intraportal Transplantation. Am J Transplant (2020) 20:2703–14. doi: 10.1111/ajt.15958

  • CrossRef
  • Google Scholar

• 125

  YaoMDomogatskayaAÅgrenNWatanabeMTokodaiKBrinesMet al. Cibinetide Protects Isolated Human Islets in a Stressful Environment and Improves Engraftment in the Perspective of Intra Portal Islet Transplantation. Cell Transplant (2021) 30:9636897211039740. doi: 10.1177/09636897211039739

  • CrossRef
  • Google Scholar

• 126

  CooperDKC. Genetically Engineered Pig Kidney Transplantation in a Brain-Dead Human Subject. Xenotransplantation (2021) 28:e12718. doi: 10.1111/xen.12718

  • CrossRef
  • Google Scholar

• 127

  Man Gets Genetically-Modified Pig Heart in World-First Transplant, in: BBC News (2022). Available at: https://www.bbc.com/news/world-us-canada-59944889 (Accessed January 11, 2022).

  • Google Scholar