Immunological Consequences of In Utero Exposure to Foreign Antigens

doi:10.3389/fimmu.2021.638435

Review

. 2021 Apr 15:12:638435.

doi: 10.3389/fimmu.2021.638435. eCollection 2021.

Immunological Consequences of In Utero Exposure to Foreign Antigens

Jeng-Chang Chen¹

Affiliations

PMID: 33936052
PMCID: PMC8082100
DOI: 10.3389/fimmu.2021.638435

Review

Immunological Consequences of In Utero Exposure to Foreign Antigens

Jeng-Chang Chen. Front Immunol. 2021.

. 2021 Apr 15:12:638435.

doi: 10.3389/fimmu.2021.638435. eCollection 2021.

Author

Jeng-Chang Chen¹

Affiliation

¹ Department of Surgery, Chang Gung Children's Hospital, College of Medicine, Chang Gung University, Taoyuan, Taiwan.

PMID: 33936052
PMCID: PMC8082100
DOI: 10.3389/fimmu.2021.638435

Abstract

Immunologic tolerance refers to a state of immune nonreactivity specific to particular antigens as an important issue in the field of transplantation and the management of autoimmune diseases. Tolerance conceptually originated from Owen's observation of blood cell sharing in twin calves. Owen's conceptual framework subsequently constituted the backbone of Medawar's "actively acquired tolerance" as the major tenet of modern immunology. Based upon this knowledge, the delivery of genetically distinct hematopoietic stem cells into pre-immune fetuses represented a novel and unique approach to their engraftment without the requirement of myeloablation or immunosuppression. It might also make fetal recipients commit donor alloantigens to memory of their patterns as "self" so as to create a state of donor-specific tolerance. Over the years, the effort made experimentally or clinically toward in utero marrow transplantation could not reliably yield sufficient hematopoietic chimerism for curing candidate diseases as anticipated, nor did allogeneic graft tolerance universally develop as envisaged by Medawar following in utero exposure to various forms of alloantigens from exosomes, lymphocytes or marrow cells. Enduring graft tolerance was only conditional on a state of significant hematopoietic chimerism conferred by marrow inocula. Notably, fetal exposure to ovalbumin, oncoprotein and microbial antigens did not elicit immune tolerance, but instead triggered an event of sensitization to the antigens inoculated. These fetal immunogenic events might be clinically relevant to prenatal imprinting of atopy, immune surveillance against developmental tumorigenesis, and prenatal immunization against infectious diseases. Briefly, the immunological consequences of fetal exposure to foreign antigens could be tolerogenic or immunogenic, relying upon the type or nature of antigens introduced. Thus, the classical school of "actively acquired tolerance" might oversimplify the interactions between developing fetal immune system and antigens. Such interactions might rely upon fetal macrophages, which showed up earlier than lymphocytes and were competent to phagocytose foreign antigens so as to bridge toward antigen-specific adaptive immunity later on in life. Thus, innate fetal macrophages may be the potential basis for exploring how the immunological outcome of fetal exposure to foreign antigens is determined to improve the likelihood and reliability of manipulating fetal immune system toward tolerization or immunization to antigens.

Keywords: alloantigen; bone marrow transplantation; fetus; hematopoietic chimerism; immune tolerance; in utero exposure; macrophage; sensitization.

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Conflict of interest statement

The author declares that the research was conducted in the absence of any commercial or financial relationships that could be constructed as a potential conflict of interest.

Figures

**Figure 1**
Skin graft tolerance in a state of hematopoietic chimerism. Following *in utero* injection of C57BL/6 (H-2^b) BMCs into gestational day 14 FVB/N (H-2^q) fetuses, skin transplantation was performed in a representative mixed chimera with 5.63% peripheral blood cell chimerism at 1 month old. The image taken at 5 months old showed that syngeneic FVB/N (arrow) and donor C57BL/6 (black hair) skin grafts were well accepted with good hair growth, but third-party C3H (H-2^k, arrowhead) skin had been rejected with a scar. It supported a state of donor-specific immune tolerance.

**Figure 2**
Anaphylaxis in FVB/N mice prenatally exposed to ovalbumin. Gestational day 14 FVB/N fetuses were intraperitoneally exposed to free ovalbumin peptides. Postnatally, they received intraperitoneal ovalbumin re-challenge. **(A)** Within 10-15 minutes, mice developed limb weakness and **(B)** cyanotic nose, ears, **(C)** genitalia, feet and tail as compared with the normal control (right mouse). Subsequently, the mice presented with shallow breathing, and finally succumbed to anaphylaxis. Postnatal anaphylaxis indicated a prior sensitization event in fetal life.

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References

1. Owen RD. Immunogenetic consequences of vascular anastomoses between bovine twins. Science (1945) 102:400–1. 10.1126/science.102.2651.400 - DOI - PubMed
1. Anderson D, Billingham RE, Lampkin GH, Medawar PB. The use of skin grafting to distinguish between monozygotic and dizygotic twins in cattle. Heredity (1951) 5:379–97. 10.1038/hdy.1951.38 - DOI
1. Billingham RE, Lampkin GH, Medawar PB, Williams HL. Tolerance to homografts, twin diagnosis, and the freemartin condition in cattle. Heredity (1952) 6:201–12. 10.1038/hdy.1952.20 - DOI
1. Billingham RE, Brent L, Medawar PB. Actively acquired tolerance of foreign cells. Nature (1953) 172:603–6. 10.1038/172603a0 - DOI - PubMed
1. Hodgkin PD, Heath WR, Baxter AG. The clonal selection theory: 50 years since the revolution. Nat Immunol (2007) 8:1019–26. 10.1038/ni1007-1019 - DOI - PubMed

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[1] Owen RD. Immunogenetic consequences of vascular anastomoses between bovine twins. Science (1945) 102:400–1. 10.1126/science.102.2651.400 - DOI - PubMed

[2] Owen RD. Immunogenetic consequences of vascular anastomoses between bovine twins. Science (1945) 102:400–1. 10.1126/science.102.2651.400 - DOI - PubMed

[3] Anderson D, Billingham RE, Lampkin GH, Medawar PB. The use of skin grafting to distinguish between monozygotic and dizygotic twins in cattle. Heredity (1951) 5:379–97. 10.1038/hdy.1951.38 - DOI

[4] Anderson D, Billingham RE, Lampkin GH, Medawar PB. The use of skin grafting to distinguish between monozygotic and dizygotic twins in cattle. Heredity (1951) 5:379–97. 10.1038/hdy.1951.38 - DOI

[5] Billingham RE, Lampkin GH, Medawar PB, Williams HL. Tolerance to homografts, twin diagnosis, and the freemartin condition in cattle. Heredity (1952) 6:201–12. 10.1038/hdy.1952.20 - DOI

[6] Billingham RE, Lampkin GH, Medawar PB, Williams HL. Tolerance to homografts, twin diagnosis, and the freemartin condition in cattle. Heredity (1952) 6:201–12. 10.1038/hdy.1952.20 - DOI

[7] Billingham RE, Brent L, Medawar PB. Actively acquired tolerance of foreign cells. Nature (1953) 172:603–6. 10.1038/172603a0 - DOI - PubMed

[8] Billingham RE, Brent L, Medawar PB. Actively acquired tolerance of foreign cells. Nature (1953) 172:603–6. 10.1038/172603a0 - DOI - PubMed

[9] Hodgkin PD, Heath WR, Baxter AG. The clonal selection theory: 50 years since the revolution. Nat Immunol (2007) 8:1019–26. 10.1038/ni1007-1019 - DOI - PubMed

[10] Hodgkin PD, Heath WR, Baxter AG. The clonal selection theory: 50 years since the revolution. Nat Immunol (2007) 8:1019–26. 10.1038/ni1007-1019 - DOI - PubMed

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Immunological Consequences of In Utero Exposure to Foreign Antigens

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Immunological Consequences of In Utero Exposure to Foreign Antigens

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