Immunotherapies based on macrophage reprogramming in periodontitis and apical periodontitis

David González-Quintanilla; Sebastián Castro-Saavedra; María José Bordagaray; Joaquín Lucero-Mora; Rolando Vernal; Andrea Paula-Lima; Alejandra Fernández; Marcela Hernández

doi:10.1007/s00784-026-06918-4

Immunotherapies based on macrophage reprogramming in periodontitis and apical periodontitis

David González-Quintanilla
, Sebastián Castro-Saavedra
, María José Bordagaray
, Joaquín Lucero-Mora
, Rolando Vernal
, Andrea Paula-Lima
, Alejandra Fernández
, Marcela Hernández^*

^*Corresponding author for this work

Research output: Contribution to journal › Review article › peer-review

Abstract

Introduction: Periodontitis and apical periodontitis (AP) are characterized by biofilm-driven, immune-mediated bone destruction. Macrophages orchestrate the immune imbalance, where the M1/M2 polarization axis is critical for tissue homeostasis. Aim: To review preclinical strategies for macrophage reprogramming-based immunotherapies in periodontitis and AP. Methods: A literature search in Web of Science (last 10 years) identified original in vivo and complementary in vitro studies evaluating interventions targeting macrophage polarization. Eligible studies reported M1 markers (CD80, CD8, and/or iNOS) and M2 markers (CD163, CD206, and/or Arg-1) in relation to inflammatory modulation and regenerative outcomes. Results: Fifteen studies met the criteria. In periodontitis, local therapeutic strategies such as bioactive cytokines (CCL2, IL-37), inhibition of extracellular matrix proteins (FBLN3), functionalized biomaterials (Se-nHA/PC microspheres, Q@MPDA nanoparticles), MSC-derived exosomes, regulatory miRNAs (miR-126), pharmacological agents (glipizide, apabetalone), and adoptive M2 transfer demonstrated M2 polarization. In AP, systemically administered M2-derived extracellular vesicles, pharmacological agents (DMOG, Stattic, azithromycin), and blockade of Gremlin-1 are associated with M2 phenotypes. All reduced alveolar bone loss, osteoclast activity, and pro-inflammatory mediators, while favoring reparative responses. Mechanistically, effects were mediated through MAPKs, PI3K/Akt/HIF-1α, STAT3, and NF-κB pathways. Conclusions: Current evidence highlights macrophage reprogramming toward an M2 phenotype as a promising adjunctive strategy for periodontitis and AP. Delivered locally or systemically, these interventions dampen M1-driven inflammation and enhance regeneration, though validation in orthotopic models and translational studies remains necessary. Clinical relevance: Immunotherapeutic approaches targeting macrophage polarization could complement conventional biofilm control with emphasis on regenerative periodontics and endodontic procedures, opening new avenues for biologically driven, patient-centered therapies.

Original language	English
Article number	234
Journal	Clinical Oral Investigations
Volume	30
Issue number	6
DOIs	https://doi.org/10.1007/s00784-026-06918-4
State	Published - Jun 2026
Externally published	Yes

Bibliographical note

Publisher Copyright:
© The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature 2026.

Keywords

Apical periodontitis
Immunomodulation
Immunotherapy
Macrophages
Periodontitis

Access to Document

10.1007/s00784-026-06918-4

Cite this

@article{8e509a9a5b844589bc670c23400e6cdf,

title = "Immunotherapies based on macrophage reprogramming in periodontitis and apical periodontitis",

abstract = "Introduction: Periodontitis and apical periodontitis (AP) are characterized by biofilm-driven, immune-mediated bone destruction. Macrophages orchestrate the immune imbalance, where the M1/M2 polarization axis is critical for tissue homeostasis. Aim: To review preclinical strategies for macrophage reprogramming-based immunotherapies in periodontitis and AP. Methods: A literature search in Web of Science (last 10 years) identified original in vivo and complementary in vitro studies evaluating interventions targeting macrophage polarization. Eligible studies reported M1 markers (CD80, CD8, and/or iNOS) and M2 markers (CD163, CD206, and/or Arg-1) in relation to inflammatory modulation and regenerative outcomes. Results: Fifteen studies met the criteria. In periodontitis, local therapeutic strategies such as bioactive cytokines (CCL2, IL-37), inhibition of extracellular matrix proteins (FBLN3), functionalized biomaterials (Se-nHA/PC microspheres, Q@MPDA nanoparticles), MSC-derived exosomes, regulatory miRNAs (miR-126), pharmacological agents (glipizide, apabetalone), and adoptive M2 transfer demonstrated M2 polarization. In AP, systemically administered M2-derived extracellular vesicles, pharmacological agents (DMOG, Stattic, azithromycin), and blockade of Gremlin-1 are associated with M2 phenotypes. All reduced alveolar bone loss, osteoclast activity, and pro-inflammatory mediators, while favoring reparative responses. Mechanistically, effects were mediated through MAPKs, PI3K/Akt/HIF-1α, STAT3, and NF-κB pathways. Conclusions: Current evidence highlights macrophage reprogramming toward an M2 phenotype as a promising adjunctive strategy for periodontitis and AP. Delivered locally or systemically, these interventions dampen M1-driven inflammation and enhance regeneration, though validation in orthotopic models and translational studies remains necessary. Clinical relevance: Immunotherapeutic approaches targeting macrophage polarization could complement conventional biofilm control with emphasis on regenerative periodontics and endodontic procedures, opening new avenues for biologically driven, patient-centered therapies.",

keywords = "Apical periodontitis, Immunomodulation, Immunotherapy, Macrophages, Periodontitis",

author = "David Gonz{\'a}lez-Quintanilla and Sebasti{\'a}n Castro-Saavedra and Bordagaray, \{Mar{\'i}a Jos{\'e}\} and Joaqu{\'i}n Lucero-Mora and Rolando Vernal and Andrea Paula-Lima and Alejandra Fern{\'a}ndez and Marcela Hern{\'a}ndez",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature 2026.",

year = "2026",

month = jun,

doi = "10.1007/s00784-026-06918-4",

language = "English",

volume = "30",

journal = "Clinical Oral Investigations",

issn = "1432-6981",

publisher = "Springer Verlag",

number = "6",

}

TY - JOUR

T1 - Immunotherapies based on macrophage reprogramming in periodontitis and apical periodontitis

AU - González-Quintanilla, David

AU - Castro-Saavedra, Sebastián

AU - Bordagaray, María José

AU - Lucero-Mora, Joaquín

AU - Vernal, Rolando

AU - Paula-Lima, Andrea

AU - Fernández, Alejandra

AU - Hernández, Marcela

N1 - Publisher Copyright: © The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature 2026.

PY - 2026/6

Y1 - 2026/6

N2 - Introduction: Periodontitis and apical periodontitis (AP) are characterized by biofilm-driven, immune-mediated bone destruction. Macrophages orchestrate the immune imbalance, where the M1/M2 polarization axis is critical for tissue homeostasis. Aim: To review preclinical strategies for macrophage reprogramming-based immunotherapies in periodontitis and AP. Methods: A literature search in Web of Science (last 10 years) identified original in vivo and complementary in vitro studies evaluating interventions targeting macrophage polarization. Eligible studies reported M1 markers (CD80, CD8, and/or iNOS) and M2 markers (CD163, CD206, and/or Arg-1) in relation to inflammatory modulation and regenerative outcomes. Results: Fifteen studies met the criteria. In periodontitis, local therapeutic strategies such as bioactive cytokines (CCL2, IL-37), inhibition of extracellular matrix proteins (FBLN3), functionalized biomaterials (Se-nHA/PC microspheres, Q@MPDA nanoparticles), MSC-derived exosomes, regulatory miRNAs (miR-126), pharmacological agents (glipizide, apabetalone), and adoptive M2 transfer demonstrated M2 polarization. In AP, systemically administered M2-derived extracellular vesicles, pharmacological agents (DMOG, Stattic, azithromycin), and blockade of Gremlin-1 are associated with M2 phenotypes. All reduced alveolar bone loss, osteoclast activity, and pro-inflammatory mediators, while favoring reparative responses. Mechanistically, effects were mediated through MAPKs, PI3K/Akt/HIF-1α, STAT3, and NF-κB pathways. Conclusions: Current evidence highlights macrophage reprogramming toward an M2 phenotype as a promising adjunctive strategy for periodontitis and AP. Delivered locally or systemically, these interventions dampen M1-driven inflammation and enhance regeneration, though validation in orthotopic models and translational studies remains necessary. Clinical relevance: Immunotherapeutic approaches targeting macrophage polarization could complement conventional biofilm control with emphasis on regenerative periodontics and endodontic procedures, opening new avenues for biologically driven, patient-centered therapies.

AB - Introduction: Periodontitis and apical periodontitis (AP) are characterized by biofilm-driven, immune-mediated bone destruction. Macrophages orchestrate the immune imbalance, where the M1/M2 polarization axis is critical for tissue homeostasis. Aim: To review preclinical strategies for macrophage reprogramming-based immunotherapies in periodontitis and AP. Methods: A literature search in Web of Science (last 10 years) identified original in vivo and complementary in vitro studies evaluating interventions targeting macrophage polarization. Eligible studies reported M1 markers (CD80, CD8, and/or iNOS) and M2 markers (CD163, CD206, and/or Arg-1) in relation to inflammatory modulation and regenerative outcomes. Results: Fifteen studies met the criteria. In periodontitis, local therapeutic strategies such as bioactive cytokines (CCL2, IL-37), inhibition of extracellular matrix proteins (FBLN3), functionalized biomaterials (Se-nHA/PC microspheres, Q@MPDA nanoparticles), MSC-derived exosomes, regulatory miRNAs (miR-126), pharmacological agents (glipizide, apabetalone), and adoptive M2 transfer demonstrated M2 polarization. In AP, systemically administered M2-derived extracellular vesicles, pharmacological agents (DMOG, Stattic, azithromycin), and blockade of Gremlin-1 are associated with M2 phenotypes. All reduced alveolar bone loss, osteoclast activity, and pro-inflammatory mediators, while favoring reparative responses. Mechanistically, effects were mediated through MAPKs, PI3K/Akt/HIF-1α, STAT3, and NF-κB pathways. Conclusions: Current evidence highlights macrophage reprogramming toward an M2 phenotype as a promising adjunctive strategy for periodontitis and AP. Delivered locally or systemically, these interventions dampen M1-driven inflammation and enhance regeneration, though validation in orthotopic models and translational studies remains necessary. Clinical relevance: Immunotherapeutic approaches targeting macrophage polarization could complement conventional biofilm control with emphasis on regenerative periodontics and endodontic procedures, opening new avenues for biologically driven, patient-centered therapies.

KW - Apical periodontitis

KW - Immunomodulation

KW - Immunotherapy

KW - Macrophages

KW - Periodontitis

UR - https://www.scopus.com/pages/publications/105039008687

U2 - 10.1007/s00784-026-06918-4

DO - 10.1007/s00784-026-06918-4

M3 - Review article

C2 - 42133106

AN - SCOPUS:105039008687

SN - 1432-6981

VL - 30

JO - Clinical Oral Investigations

JF - Clinical Oral Investigations

IS - 6

M1 - 234

ER -

Immunotherapies based on macrophage reprogramming in periodontitis and apical periodontitis

Abstract

Bibliographical note

Keywords

Access to Document

Other files and links

Fingerprint

Cite this