Targeting lymphatic vessels enhances bone regeneration by augmenting osteoclast activity in mouse models of amputation

Neda Vishlaghi; Trisha K. Ghotra; Monisha Mittal; Ji Hae L. Choi; Sneha Korlakunta; Mingquan Yan; Janna L. Crossley; Danielle Griswold-Wheeler; Elnaz Ghotbi; Conan Juan; Shiri Gur-Cohen; Babak Mehrara; David A. Brown; Michael T. Dellinger; Lindsay A. Dawson; Benjamin Levi

doi:10.1172/JCI191906

Targeting lymphatic vessels enhances bone regeneration by augmenting osteoclast activity in mouse models of amputation

Neda Vishlaghi, Trisha K. Ghotra, Monisha Mittal, Ji Hae L. Choi, Sneha Korlakunta, Mingquan Yan, Janna L. Crossley, Danielle Griswold-Wheeler, Elnaz Ghotbi, Conan Juan, Shiri Gur-Cohen, Babak Mehrara, David A. Brown, Michael T. Dellinger, Lindsay A. Dawson, Benjamin Levi

Surgery

Research output: Contribution to journal › Article › peer-review

Abstract

Although mammals generally demonstrate limited regenerative capacity compared with amphibians, the digit tip retains remarkable regenerative potential, providing a useful model to study successful mammalian regeneration. This process involves coordinated immune cell activity, vascular remodeling, and tissue reconstruction, yet the molecular checkpoints controlling regenerative versus fibrotic outcomes remain poorly understood. In mammals, regeneration of the digit tip (P3) proceeds through myeloid cell migration, early osteoclast-mediated osteolysis of the distal bone, and subsequent blastema-mediated regeneration. Here we test the hypothesis that lymphatic vessels regulate regenerative capacity by modulating local immune cell dynamics and osteoclast function. Using a lymphatic system-specific reporter line, we discovered that lymphatic vessels grow toward the nail region from the ventral side of the digit during quiescence and after amputation. These lymphatics closely surround, but do not invade, the native or regenerated bone. Unexpectedly, genetic, pharmacological, and surgical inhibition of lymphangiogenesis accelerated early osteolysis through enhanced transition of myeloid cells to osteoclasts, resulting in faster and more robust regeneration. These findings reveal a mechanism linking lymphatic vessel, immune regulation, and bone remodeling, suggesting that targeted manipulation of lymphatics dynamics may enhance regenerative outcomes after musculoskeletal injury.

Original language	English
Journal	Journal of Clinical Investigation
Volume	136
Issue number	3
DOIs	https://doi.org/10.1172/JCI191906
State	Published - 2 Feb 2026

Keywords

Bone biology
Osteoclast/osteoblast biology
Vascular biology

Access to Document

10.1172/JCI191906

Cite this

Vishlaghi, N., Ghotra, T. K., Mittal, M., Choi, J. H. L., Korlakunta, S., Yan, M., Crossley, J. L., Griswold-Wheeler, D., Ghotbi, E., Juan, C., Gur-Cohen, S., Mehrara, B., Brown, D. A., Dellinger, M. T., Dawson, L. A., & Levi, B. (2026). Targeting lymphatic vessels enhances bone regeneration by augmenting osteoclast activity in mouse models of amputation. Journal of Clinical Investigation, 136(3). https://doi.org/10.1172/JCI191906

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title = "Targeting lymphatic vessels enhances bone regeneration by augmenting osteoclast activity in mouse models of amputation",

abstract = "Although mammals generally demonstrate limited regenerative capacity compared with amphibians, the digit tip retains remarkable regenerative potential, providing a useful model to study successful mammalian regeneration. This process involves coordinated immune cell activity, vascular remodeling, and tissue reconstruction, yet the molecular checkpoints controlling regenerative versus fibrotic outcomes remain poorly understood. In mammals, regeneration of the digit tip (P3) proceeds through myeloid cell migration, early osteoclast-mediated osteolysis of the distal bone, and subsequent blastema-mediated regeneration. Here we test the hypothesis that lymphatic vessels regulate regenerative capacity by modulating local immune cell dynamics and osteoclast function. Using a lymphatic system-specific reporter line, we discovered that lymphatic vessels grow toward the nail region from the ventral side of the digit during quiescence and after amputation. These lymphatics closely surround, but do not invade, the native or regenerated bone. Unexpectedly, genetic, pharmacological, and surgical inhibition of lymphangiogenesis accelerated early osteolysis through enhanced transition of myeloid cells to osteoclasts, resulting in faster and more robust regeneration. These findings reveal a mechanism linking lymphatic vessel, immune regulation, and bone remodeling, suggesting that targeted manipulation of lymphatics dynamics may enhance regenerative outcomes after musculoskeletal injury.",

keywords = "Bone biology, Osteoclast/osteoblast biology, Vascular biology",

author = "Neda Vishlaghi and Ghotra, {Trisha K.} and Monisha Mittal and Choi, {Ji Hae L.} and Sneha Korlakunta and Mingquan Yan and Crossley, {Janna L.} and Danielle Griswold-Wheeler and Elnaz Ghotbi and Conan Juan and Shiri Gur-Cohen and Babak Mehrara and Brown, {David A.} and Dellinger, {Michael T.} and Dawson, {Lindsay A.} and Benjamin Levi",

year = "2026",

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doi = "10.1172/JCI191906",

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Vishlaghi, N, Ghotra, TK, Mittal, M, Choi, JHL, Korlakunta, S, Yan, M, Crossley, JL, Griswold-Wheeler, D, Ghotbi, E, Juan, C, Gur-Cohen, S, Mehrara, B, Brown, DA, Dellinger, MT, Dawson, LA & Levi, B 2026, 'Targeting lymphatic vessels enhances bone regeneration by augmenting osteoclast activity in mouse models of amputation', Journal of Clinical Investigation, vol. 136, no. 3. https://doi.org/10.1172/JCI191906

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T1 - Targeting lymphatic vessels enhances bone regeneration by augmenting osteoclast activity in mouse models of amputation

AU - Vishlaghi, Neda

AU - Ghotra, Trisha K.

AU - Mittal, Monisha

AU - Choi, Ji Hae L.

AU - Korlakunta, Sneha

AU - Yan, Mingquan

AU - Crossley, Janna L.

AU - Griswold-Wheeler, Danielle

AU - Ghotbi, Elnaz

AU - Juan, Conan

AU - Gur-Cohen, Shiri

AU - Mehrara, Babak

AU - Brown, David A.

AU - Dellinger, Michael T.

AU - Dawson, Lindsay A.

AU - Levi, Benjamin

PY - 2026/2/2

Y1 - 2026/2/2

N2 - Although mammals generally demonstrate limited regenerative capacity compared with amphibians, the digit tip retains remarkable regenerative potential, providing a useful model to study successful mammalian regeneration. This process involves coordinated immune cell activity, vascular remodeling, and tissue reconstruction, yet the molecular checkpoints controlling regenerative versus fibrotic outcomes remain poorly understood. In mammals, regeneration of the digit tip (P3) proceeds through myeloid cell migration, early osteoclast-mediated osteolysis of the distal bone, and subsequent blastema-mediated regeneration. Here we test the hypothesis that lymphatic vessels regulate regenerative capacity by modulating local immune cell dynamics and osteoclast function. Using a lymphatic system-specific reporter line, we discovered that lymphatic vessels grow toward the nail region from the ventral side of the digit during quiescence and after amputation. These lymphatics closely surround, but do not invade, the native or regenerated bone. Unexpectedly, genetic, pharmacological, and surgical inhibition of lymphangiogenesis accelerated early osteolysis through enhanced transition of myeloid cells to osteoclasts, resulting in faster and more robust regeneration. These findings reveal a mechanism linking lymphatic vessel, immune regulation, and bone remodeling, suggesting that targeted manipulation of lymphatics dynamics may enhance regenerative outcomes after musculoskeletal injury.

AB - Although mammals generally demonstrate limited regenerative capacity compared with amphibians, the digit tip retains remarkable regenerative potential, providing a useful model to study successful mammalian regeneration. This process involves coordinated immune cell activity, vascular remodeling, and tissue reconstruction, yet the molecular checkpoints controlling regenerative versus fibrotic outcomes remain poorly understood. In mammals, regeneration of the digit tip (P3) proceeds through myeloid cell migration, early osteoclast-mediated osteolysis of the distal bone, and subsequent blastema-mediated regeneration. Here we test the hypothesis that lymphatic vessels regulate regenerative capacity by modulating local immune cell dynamics and osteoclast function. Using a lymphatic system-specific reporter line, we discovered that lymphatic vessels grow toward the nail region from the ventral side of the digit during quiescence and after amputation. These lymphatics closely surround, but do not invade, the native or regenerated bone. Unexpectedly, genetic, pharmacological, and surgical inhibition of lymphangiogenesis accelerated early osteolysis through enhanced transition of myeloid cells to osteoclasts, resulting in faster and more robust regeneration. These findings reveal a mechanism linking lymphatic vessel, immune regulation, and bone remodeling, suggesting that targeted manipulation of lymphatics dynamics may enhance regenerative outcomes after musculoskeletal injury.

KW - Bone biology

KW - Osteoclast/osteoblast biology

KW - Vascular biology

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