Reduced Bone Mass in Collagen Prolyl 4-Hydroxylase P4ha1 +/-; P4ha2 -/- Compound Mutant Mice

Jussi-Pekka Tolonen; Antti M Salo; Mikko Finnilä; Ellinoora Aro; Emma Karjalainen; Veli-Pekka Ronkainen; Kati Drushinin; Christophe Merceron; Valerio Izzi; Ernestina Schipani; Johanna Myllyharju

doi:10.1002/jbm4.10630

Reduced Bone Mass in Collagen Prolyl 4-Hydroxylase P4ha1 ^+/-; P4ha2 ^-/- Compound Mutant Mice

JBMR Plus. 2022 May 9;6(6):e10630. doi: 10.1002/jbm4.10630. eCollection 2022 Jun.

Authors

Jussi-Pekka Tolonen^{1

2

3}, Antti M Salo^{1

2

3}, Mikko Finnilä⁴, Ellinoora Aro^{1

2

3}, Emma Karjalainen^{1

2

3}, Veli-Pekka Ronkainen², Kati Drushinin^{1

2

3}, Christophe Merceron⁵, Valerio Izzi^{1

3

6

7}, Ernestina Schipani^{5

8}, Johanna Myllyharju^{1

2

3}

Affiliations

¹ Oulu Center for Cell-Matrix Research University of Oulu Oulu Finland.
² Biocenter Oulu University of Oulu Oulu Finland.
³ Faculty of Biochemistry and Molecular Medicine University of Oulu Oulu Finland.
⁴ Research Unit of Medical Imaging, Physics and Technology, Faculty of Medicine University of Oulu Oulu Finland.
⁵ Departments of Orthopaedic Surgery, Medicine, and Cell and Developmental Biology University of Michigan School of Medicine Ann Arbor MI USA.
⁶ Research Unit of Biomedicine, Faculty of Medicine University of Oulu Oulu Finland.
⁷ Finnish Cancer Institute Helsinki Finland.
⁸ Present address: McKay Laboratory, Department of Orthopedic Surgery University of Pennsylvania-Perelman Medical School Philadelphia PA USA.

Abstract

Proper deposition of the extracellular matrix and its major components, the collagens, is essential for endochondral ossification and bone mass accrual. Collagen prolyl 4-hydroxylases (C-P4Hs) hydroxylate proline residues in the -X-Pro-Gly- repeats of all known collagen types. Their product, 4-hydroxyproline, is essential for correct folding and thermal stability of the triple-helical collagen molecules in physiological body temperatures. We have previously shown that inactivation of the mouse P4ha1 gene, which codes for the catalytic α subunit of the major C-P4H isoform, is embryonic lethal, whereas inactivation of the P4ha2 gene produced only a minor phenotype. Instead, mice with a haploinsufficiency of the P4ha1 gene combined with a homozygous deletion of the P4ha2 gene present with a moderate chondrodysplasia due to transient cell death of the growth plate chondrocytes. Here, to further characterize the bone phenotype of the P4ha1 ^+/-; P4ha2 ^-/- mice, we have carried out gene expression analyses at whole-tissue and single-cell levels, biochemical analyses, microcomputed tomography, histomorphometric analyses, and second harmonic generation microscopy to show that C-P4H α subunit expression peaks early and that the C-P4H deficiency leads to reduced collagen amount, a reduced rate of bone formation, and a loss of trabecular and cortical bone volume in the long bones. The total osteoblast number in the proximal P4ha1 ^+/-; P4ha2 ^-/- tibia and the C-P4H activity in primary P4ha1 ^+/-; P4ha2 ^-/- osteoblasts were reduced, whereas the population of osteoprogenitor colony-forming unit fibroblasts was increased in the P4ha1 ^+/-; P4ha2 ^-/- marrow. Thus, the P4ha1 ^+/-; P4ha2 ^-/- mouse model recapitulates key aspects of a recently recognized congenital connective tissue disorder with short stature and bone dysplasia caused by biallelic variants of the human P4HA1 gene. Altogether, the data demonstrate the allele dose-dependent importance of the C-P4Hs to the developing organism and a threshold effect of C-P4H activity in the proper production of bone matrix. © 2022 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research.

Keywords: BONE HISTOMORPHOMETRY; BONE μCT; COLLAGEN; GENETIC ANIMAL MODELS; OSTEOBLASTS.