Next Article in Journal
Routine Laboratory Markers as Incremental Predictors Beyond OSTA for Dual-Energy X-Ray Absorptiometry-Defined Osteoporosis: Internal Validation in a Referral Cohort
Previous Article in Journal
Predictors of Diagnostic Yield in Shape-Sensing Robotic-Assisted Bronchoscopy (ssRAB): A Retrospective Single-Center Study
Previous Article in Special Issue
Diagnostic Challenge: An Extremely Rare Case of Intra-Articular Myopericytoma of the Knee
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
Diagnostics
Volume 16
Issue 13
10.3390/diagnostics16131955
diagnostics-logo
Submit to this Journal Review for this Journal Propose a Special Issue
Article Menu

Article Menu

share Share announcement Help format_quote Cite
first_page
settings
Order Article Reprints
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Article

Multiple Ossification Centers of the Pubic Bone as a Supportive Radiographic Feature for COL2A1-Related Congenital Spondyloepiphyseal Dysplasia

by
Vladimir Kenis
1,*,
Tatiana Markova
2,
Evgeniy Melchenko
1 and
Daria Gorodilova
2
1
H. Turner National Medical Research Center for Children’s Orthopedics and Trauma Surgery, Parkovaya 64–68, Pushkin, 196603 Saint-Petersburg, Russia
2
Research Centre for Medical Genetics, Moskvorechye St., 1, 115522 Moscow, Russia
*
Author to whom correspondence should be addressed.
Diagnostics 2026, 16(13), 1955; https://doi.org/10.3390/diagnostics16131955 (registering DOI)
Submission received: 4 May 2026 / Revised: 20 June 2026 / Accepted: 21 June 2026 / Published: 23 June 2026
(This article belongs to the Special Issue Advanced Imaging for Diagnosis and Management of Musculoskeletal Disorders)
Browse Figures
Versions Notes

Abstract

Background/Objectives: During analysis of patients with genetically confirmed COL2A1-related skeletal dysplasias, we observed an unusual ossification pattern of the superior pubic ramus characterized by multiple ossification centers—a phenomenon not previously reported in this context. The study aimed to determine the consistency and frequency of multiple ossification centers of the superior pubic ramus in patients with COL2A1-related skeletal dysplasias. Methods: We retrospectively analyzed pelvic radiographs from 135 patients with genetically confirmed pathogenic COL2A1 variants. Patients were classified into four clinical subgroups: SEDC, MED, Kniest dysplasia, and Stickler syndrome. Results: Multiple ossification centers were identified in 20 (15.5%) of the included patients, all of whom had the SEDC phenotype. The sensitivity of this radiographic sign for SEDC was 36.36%, with high specificity (99.07%) and accuracy (96.5%) compared with other COL2A1-related phenotypes and historical general population data. However, these findings require cautious interpretation given the limitations of historical control data. Conclusions: We identified an uncommon atypical ossification pattern of the superior pubic ramus that may serve as a supportive radiographic feature when interpreted in conjunction with clinical and genetic findings.

1. Introduction

Significant advances in and the increased accessibility of genetic testing have been evident in recent years. Nevertheless, clinical and radiographic evaluation remains essential for diagnosing and managing rare hereditary diseases, including skeletal dysplasias. COL2A1-associated skeletal dysplasias represent a substantial proportion of all skeletal dysplasias. Their clinical manifestations form a spectrum, ranging from the mildest, manifesting late in life (early osteoarthritis), to lethal dysplasias characterized by extreme short stature and significant anatomical defects. The clinical spectrum of COL2A1-related skeletal dysplasias, according to the 2023 revision of “Nosology of genetic skeletal disorders” includes spondyloepiphyseal dysplasia congenita [1].
Although some genotype–phenotype correlations have been identified, no recurrent variants have been consistently associated with strictly defined clinical forms within this spectrum. Instead, COL2A1-related skeletal dysplasias manifest as a continuum of clinical presentations [2].
Congenital spondyloepiphyseal dysplasia (SEDC) is a classical COL2A1-related skeletal dysplasia. In typical cases, it manifests with disproportionate short stature, abnormal epiphyses, and flattened vertebral bodies with manifestations presented at birth [3]. Key radiographic manifestations of SEDC in infancy include delayed ossification of the skeleton with absence of the ossification centers of the pubic bones and knee epiphyses, and absent ossification of the vertebral bodies of the upper cervical spine, as well as small, dorsally wedged vertebral bodies of the thoracic and lumbar spine, and delayed ossification of the sacrum. In childhood, radiographic findings include retarded ossification of the pelvis with horizontal acetabular roofs, absent or retarded ossification of the femoral head and neck, coxa vara (occasionally preserved ossification and normal angulation of the femoral neck), varying degrees of epiphyseal and metaphyseal abnormalities of the long tubular bones, and delayed appearance of the carpal and tarsal ossification centers [4].
SEDC is the prototype of the “SEDC family”, the composition of which has expanded and contracted over time with successive publications due to the description of new forms and the reclassification of previously described phenotypes [5].
Radiologic hallmarks of SEDC include delayed endochondral ossification of juxtatruncal bones, delayed ossification of thoracic and lumbar vertebral bodies (with a characteristic pear-shaped appearance), and severely delayed pubic bone ossification that is commonly not appreciated at birth. Epiphyseal ossification is also delayed, and long bones are short and broad, occasionally showing mild dumbbell deformities.
Determining the specific clinical form—not merely the genetic variant—within diseases associated with pathogenic variants in the same gene (particularly COL2A1) is important for prognosis, including the prediction of linear growth [6] and complication risk. For instance, SEDC patients have a higher risk of cervical instability and scoliosis, while Stickler syndrome patients are more prone to ophthalmological and auditory disorders. This information is valuable for parents and caregivers to facilitate prevention and early detection [7].
Radiographs of the pelvis, which Gajarajulu et al. called “a window to skeletal dysplasias” [8], are one of the most important sources of diagnostic information [9].
A number of radiographic features of pelvic bones ossification have been described in patients with COL2A1-related skeletal dysplasias. In particular, SEDC is characterized by short, broad pelvic wings with horizontal acetabular roofs and narrow sciatic notches [10].
Abnormal, delayed or, depending on the age, absent ossification of the pubic bones is known in SEDC, as well as in cleidocranial dysostosis, achondrogenesis, hypochondrogenesis, Sjogren–Larssen syndrome, Wolf syndrome, and congenital spondyloepiphyseal dysplasia [8,9,11,12,13].
Apart from delayed ossification, other features of superior pubic ramus ossification in SEDC and COL2A1-related skeletal dysplasias have not been described. While analyzing data from a large cohort of patients with genetically confirmed COL2A1-related skeletal dysplasias, we observed an unusual ossification pattern in several patients with SEDC, namely multiple ossification centers.
This phenomenon has not been previously noted in published studies on COL2A1-related skeletal dysplasias. A literature search indicates that this finding is rare and that data on this topic are extremely limited. Extensive studies of pelvic imaging in newborns [14] and children [15] have not reported additional pubic bone ossification centers.
The only publication directly addressing radiographic patterns of pubic bone ossification in children and noting the possibility of multiple ossification centers is the landmark 1956 study by Caffey and Madell [16]. They analyzed pelvic radiographs from 1286 randomly selected newborns, classifying the primary pubic ossification center at birth into three types based on shape and extent. A fourth type encompassed all cases with two or more ossification centers in one or both pubic bones. Multiple ossification centers were identified in 19 of the 1286 infants (1.5%). The most common radiographic manifestation was a vertical radiolucent strip, which in several cases resembled a fracture line. The age of closure varied, occurring as early as 5 months and as late as 1 year.
As Perez-Rossello et al. noted [17], curiously, this distinctive normal variant has received scant mention in the literature. Their study represents the second (after 50 years) and to date the last investigation of this phenomenon, albeit from the perspective of differential diagnosis with child abuse.
Therefore, we hypothesized that this ossification pattern may be more common in patients with COL2A1-related skeletal dysplasias. The aim of this study was to determine the consistency and frequency of multiple ossification centers of the superior pubic ramus in patients with COL2A1-related skeletal dysplasias, specifically comparing SEDC with other clinical forms.

2. Materials and Methods

We conducted a retrospective analysis of pelvic radiographs of 135 patients with various skeletal dysplasias with genetically confirmed pathogenic COL2A1 variants. The study utilized a database compiled through long-term collaboration by a group of geneticists and orthopedic surgeons from two tertiary academic centers in the Russian Federation. The main clinical and genetic data of this cohort were previously published [18] and subsequently supplemented.
The inclusion criteria for the study were as follows:
  • Non-lethal manifestations of skeletal dysplasia.
  • Confirmed pathogenic COL2A1 variant.
  • Availability of at least one anteroposterior pelvic radiograph with symmetrical positioning and clear visualization of both pubic bones.
  • Absence of any history of pelvic trauma or surgery.
  • Presence of two or more separate ossification centers within the superior pubic ramus, appearing as either distinct bony parts separated by a radiolucent strip (with or without marginal sclerosis) (Figure 1 and Figure 2) or as a vertical radiolucent line dividing the ramus into medial and lateral portions (Figure 3 and Figure 4). Both unilateral and bilateral findings were included.
This definition of multiple ossification centers follows that originally proposed by Caffey and Madell and Perez-Rossello et al. [16,17].
Radiographic evaluation was performed independently by two pediatric orthopedic surgeons (V.K. and E.M.) blinded to patients’ clinical and genetic diagnoses. Each reviewer assessed all available pelvic radiographs for multiple ossification centers of the superior pubic ramus as defined in the inclusion criteria. Discrepancies were recorded, and a third reviewer resolved disagreements when consensus could not be reached. Interobserver agreement was assessed using Cohen’s kappa coefficient with 95% confidence intervals. Assignment of patients to phenotypic groups was based on a combination of clinical and radiographic features provided in the fundamental “An Atlas of Genetic Disorders of Skeletal Development” [4]. The main excerpts from this atlas concerning the “classic” phenotypes (SEDC, Kniest dysplasia, Stickler syndrome) and the inclusion criteria for the SED group are presented in Supplement Table S1.
Statistical analysis was performed using StatTech software v. 4.8.0 (StatTech LLC., Kazan, Russia, https://stattech.ru, assessed on 19 June 2026). Sensitivity, specificity, and accuracy were calculated with 95% confidence intervals using the Wilson score method. Positive and negative predictive values were calculated with 95% confidence intervals using the standard formulas. Fisher’s exact test was used to compare the proportion of multiple ossification centers between SEDC and other phenotypic subgroups. A p-value < 0.05 was considered statistically significant.

3. Results

In our group of 135 patients with COL2A1-related skeletal dysplasias, pelvic radiographs were available for 129.
Multiple ossification centers were found in 20 (15.5%) of the included patients. All patients with multiple ossification centers had the SEDC phenotype (Table 1). Among the 20 patients with multiple ossification centers, 14 patients had bilateral involvement and 6 had unilateral involvement (left in 4, right in 2).
Interobserver agreement for the detection of multiple ossification centers was substantial, with Cohen’s kappa = 0.89 (95% CI: 0.78–0.96). Initial agreement between the two independent reviewers was achieved in 121 of 129 cases (93.8%). Disagreements (8 cases) were resolved by consensus discussion with the third reviewer, who was blinded to the initial independent assessments.”
Sensitivity of the sign for SEDC was 36.36% (95% CI: 23.8–50.9%), specificity 99.07% (95% CI: 94.7–99.9%), with accuracy 96.5% (95% CI: 92.4–98.5%). The positive predictive value for SEDC was 95.2% (95% CI: 74.1–99.8%) and the negative predictive value was 75.9% (95% CI: 67.8–82.5%), assuming the prevalence of SEDC within the COL2A1-related skeletal dysplasias cohort (40.7%). When comparing the SEDC group to all other phenotypes combined, the difference in the frequency of multiple ossification centers was highly significant (Fisher’s exact test, p < 0.0001).
Sensitivity and specificity of this radiographic sign were calculated for patients with COL2A1-related skeletal dysplasias and separately for SEDC compared to the general population. Since we did not have our own data on the frequency of this sign in the population, we used published data from Caffey and Madell [16]. For SEDC versus general population, sensitivity was 36.36% (95% CI: 24.2–50.1%), specificity 99.07% (95% CI: 98.4–99.5%) and accuracy 96.5% (95% CI: 94.1–98.1%).
Diagnostics 16 01955 g001
Figure 1. Anteroposterior pelvic radiograph of a 1-year-old child with SEDC showing multiple ossification centers within the superior pubic ramus, visualized as distinct bony parts (white broken lines).
Figure 1. Anteroposterior pelvic radiograph of a 1-year-old child with SEDC showing multiple ossification centers within the superior pubic ramus, visualized as distinct bony parts (white broken lines).
Diagnostics 16 01955 g001
Diagnostics 16 01955 g002
Figure 2. Enlarged anteroposterior pelvic radiographs of 18-month-old (A) and 36-month-old (B) patients with SEDC demonstrating multiple ossification centers as distinct bony parts (black arrows) separated by a radiolucent strip (white arrows).
Figure 2. Enlarged anteroposterior pelvic radiographs of 18-month-old (A) and 36-month-old (B) patients with SEDC demonstrating multiple ossification centers as distinct bony parts (black arrows) separated by a radiolucent strip (white arrows).
Diagnostics 16 01955 g002
Diagnostics 16 01955 g003
Figure 3. Anteroposterior pelvic radiograph of a 2.5-year-old patient with SEDC showing multiple ossification centers as a vertical radiolucent line dividing the ramus into medial and lateral portions (white broken lines).
Figure 3. Anteroposterior pelvic radiograph of a 2.5-year-old patient with SEDC showing multiple ossification centers as a vertical radiolucent line dividing the ramus into medial and lateral portions (white broken lines).
Diagnostics 16 01955 g003
Diagnostics 16 01955 g004
Figure 4. Enlarged anteroposterior pelvic radiographs of 3-year-old (A) and 4.5-year-old (B) patients with SEDC demonstrating bilateral (A) and unilateral (B) multiple ossification centers as vertical radiolucent lines dividing the ramus (white arrows).
Figure 4. Enlarged anteroposterior pelvic radiographs of 3-year-old (A) and 4.5-year-old (B) patients with SEDC demonstrating bilateral (A) and unilateral (B) multiple ossification centers as vertical radiolucent lines dividing the ramus (white arrows).
Diagnostics 16 01955 g004
We also analyzed the occurrence of the trait by age (Table 2).
As the data presented in Table 2 show, multiple ossification centers were observed with equal frequency in children under 1 year of age and from 1 to 10 years of age. After 10 years, we did not observe this sign.
Among the 20 patients with multiple ossification centers, genetic variants included glycine substitutions in the triple helix domain (n = 17, 85%), non-glycine substitutions (n = 1, 5%), and in-frame deletions (n = 2, 10%). This distribution was comparable to the overall SEDC cohort. No patient with multiple ossification centers had variants outside the triple helix domain, although the small sample size precludes meaningful statistical comparison.

4. Discussion

Molecular genetic analysis is currently the standard for diagnosing rare skeletal diseases. However, despite its high accuracy and increasing availability, clinical and radiographic diagnostics remain the first line of investigation [19,20]. With increasing knowledge of hereditary skeletal diseases, it has become clear that patients with this group of pathologies have virtually no pathognomonic clinical or radiographic features. Most of these features, although with varying frequencies, are clearly detectable in other diseases and even physiological conditions.
Abnormal ossification and formation of the pubic bones can be occasionally found as a developmental abnormality [21,22,23].
Therefore, defining additional diagnostic criteria enables increased diagnostic vigilance, narrowing the scope of genetic testing, and overall optimizing the diagnostic process.
Chondrification centers in the pubic bones are well developed by seven to eight weeks. The pubic ossification centers appear between five and six intrauterine months. Ossification initiates in the superior pubic ramus, anterior to the acetabulum. In the early stages of ossification the pubis is dumbbell-shaped, and is the smallest and most delicate of the pelvic elements [24].
Primary ossification centers of the pelvis initiate in utero, followed postnatally by secondary ossification at a range of locations, and these processes not complete until adulthood. This cascade of events can vary between individuals [24,25].
Postnatal ossification of the pelvis is well documented with a focus on the differential diagnosis with trauma and assessment of skeletal maturity [26,27,28].
The unusual pubic bone ossification pattern observed in children with SEDC demonstrated high specificity both relative to the general population (based on published data) and compared with patients who had other COL2A1-related skeletal dysplasias.
Numerous attempts have been made to establish clear genotype–phenotype relationships in COL2A1-related skeletal dysplasias. However, a strong, reliable prediction of phenotype has not been achieved. Notably, when describing these types, authors often use vague phrases such as ‘often associated with…’ or ‘often variants in…’ [1]. Despite the obvious patterns associated with the complex structure of the COL2A1 protein, there is clear variability, making phenotype prediction largely conditional. Nevertheless, a number of consistent phenotypic groups within this spectrum are evident. At the time w)hen classical descriptions of skeletal dysplasias were formulated, genetic confirmation was lacking, and clinicians and radiologists had to rely on careful observation. However, some less noticeable features may well have escaped attention.
For complex pathologies such as COL2A1-related skeletal dysplasias, Handa et al. proposed two principles for categorizing clinical findings [29]. First, one can categorize a particular case into a specific skeletal dysplasia family according to recognition of the overall radiologic pattern; second, one can make the diagnosis on the basis of subtle radiological findings. The first step, pattern recognition, in particular is the key to diagnosing skeletal dysplasias correctly.
The phenotypic classification of COL2A1-related skeletal dysplasias remains debated. Historically, distinct clinical syndromes were described, and later genetic analysis confirmed COL2A1 as the causative gene. Several fundamental sources of COL2A1 classification can be found in the literature. According to “Nosology of genetic skeletal disorders”, the following variants can be distinguished: COL2A1-related achondrogenesis, hypochondrogenesis, platyspondylic dysplasia, spondyloepiphyseal dysplasia congenita (SEDC), COL2A1-related spondyloepimetaphyseal dysplasia, COL2A1-related SED with metatarsal shortening, Kniest dysplasia, spondyloperipheral dysplasia, COL2A1-related Stickler syndrome, COL2A1-related dysplasia of the proximal femoral epiphyses [1]. Another well-known source of information on the phenotypes of hereditary diseases is OMIM. It distinguishes 16 phenotypes, some of which overlap with the previous source https://www.omim.org/entry/120140?search=COL2A1 (accessed on 19 June 2026). Recently, several fundamental studies have proposed their own versions of the classification of COL2A1 phenotypes and genotypes, based on clinical, radiological, and genetic principles [10,18,29]. However, clear genotype–phenotype correlations have not been established [2].
In our previous study [18], we identified 4 phenotype groups based on a combination of clinical and radiographic features. For this study, we also used this pragmatic classification into 4 phenotypes. The decision to assign a particular patient to one of the 4 groups was made by expert consensus among the authors (see “Section 2”).
This radiographic phenomenon—specific ossification of the superior pubic ramus—represents a small but potentially valuable component of the SEDC radiographic phenotype. It complements the overall diagnostic picture and may contribute to a better understanding of skeletal formation processes in health and disease.
Beyond our observation of this atypical ossification pattern, the literature emphasizes the need for differential diagnosis with child abuse [30,31]. Perez-Rossello et al. analyzed clinical, imaging, and outcome data from 14 cases (age range 1.5 to 9 months) with abnormal radiographic findings of the superior pubic ramus. In four cases (29%), the findings were classified as normal variants; in three (21%), as fractures; and in seven (50%), as indeterminate. Although SEDC is rare, its coincidence with child abuse is even less likely, though not impossible, particularly given the increasing participation of children with disabilities in sports and other activities [30,31].
Comprehensive analysis of previously published radiographs from children with COL2A1-related skeletal dysplasias is challenging, primarily due to the poor quality and unsystematized presentation of images. In later publications, however, we identified at least one clear case: a patient with SEMD Strudwick type and the p.Gly1122Arg mutation had multiple ossification centers of both superior pubic rami at age 6.8 years, although this was not noted in Terhal et al.’s article [10]. A more detailed analysis of published data may reveal additional cases, but this was not the objective of this study.
Notably, no published studies have observed multiple ossification centers in children older than one year. In our cohort, however, 10 of the 20 patients with multiple centers were between one and ten years of age. This finding suggests that the presence of multiple ossification centers beyond one year of age may have high specificity for SEDC, a finding that warrants validation in larger, controlled studies.
Our study has several limitations. First, radiographic data were collected unsystematically: pelvic radiographs were obtained at different ages and using different devices, and analysis was retrospective. Nevertheless, the clarity of the radiographic feature enabled detection in most cases. Sensitivity and specificity were assessed relative to the general population using literature data. Although this phenomenon has not been previously described in the radiographic diagnosis of COL2A1-related skeletal dysplasias, retrospective analysis of databases at skeletal dysplasia referral centers may help clarify its prevalence and quantify sensitivity and specificity.
We categorized patients with COL2A1-related skeletal dysplasias into four groups. Because the diagnostic criteria for these groups are not entirely clear, experts (orthopedic surgeons and medical geneticists with extensive experience) reached consensus on group assignment.
In this study, we did not correlate the observed phenomenon with the patients’ genotypes to avoid an excessive number of variables, as the primary objective of this article was to describe a novel radiographic feature and assess its diagnostic utility rather than to establish genotype–phenotype relationships. As previously noted, the data were obtained through the analysis of a large database of patients with SEDC. In a subsequent systematic analysis of this database, we plan to conduct a genotype–phenotype correlation for this feature. This represents an important direction for future research.
The observation that multiple ossification centers were not observed in any patient older than 10 years warrants further consideration. This finding suggests that the atypical ossification pattern represents a temporary developmental phenomenon rather than a persistent anatomical variant. In normal skeletal development, the pubic bone typically ossifies from a single primary center that appears during late fetal life and expands progressively. The presence of multiple centers in SEDC patients may reflect a more fundamental disturbance of endochondral ossification—specifically, a delay or fragmentation of the normal coalescence process. However, we cannot exclude sampling bias: older patients in our cohort had fewer radiographs available, and the retrospective design may have missed cases where the sign persisted but was not imaged. Prospective longitudinal imaging would be required to confirm the age-dependent disappearance.
Collagen type II is the major structural component of the cartilaginous anlagen of endochondrally forming bones. Pathogenic variants in COL2A1 disrupt the normal extracellular matrix structure, potentially interfering with the signaling pathways that coordinate chondrocyte differentiation and ossification center formation. The fact that multiple centers can persist until age 10 years in SEDC patients—whereas in the general population they typically fuse by 5–12 months—suggests a profound delay in the maturation of the pubic symphysis region. After age 10 years, the ossification centers ultimately fuse, indicating that the fusion process, although delayed, eventually occurs. This pattern parallels other known developmental delays in SEDC, including delayed appearance of the femoral head ossification centers and delayed carpal bone maturation.
The biological mechanisms underlying this phenomenon remain speculative. One possibility is that the abnormal collagen matrix creates physical barriers to the diffusion of ossification-promoting factors or disrupts the cell–cell communication required for coordinated ossification. Alternatively, the mechanical environment of the pubic ramus—which undergoes significant changes with weight-bearing and ambulation—may influence ossification center fusion, and the delayed motor development typical of SEDC patients (who often walk later than healthy peers) could contribute to the prolonged persistence of multiple centers. Future studies using animal models of COL2A1 mutations may help elucidate these mechanisms.
We acknowledge several important limitations regarding the use of historical control data from Caffey and Madell [16]. The imaging quality and techniques used in the mid-20th century differ substantially from modern radiographic methods, potentially affecting the detection rate of small ossification centers. The population characteristics (including nutritional status, prenatal care, and demographic factors) may differ from our contemporary Russian cohort. Radiographic interpretation standards have evolved over the past seven decades, and current observers may have different thresholds for identifying subtle radiolucencies. These factors could potentially bias our specificity estimates. However, we note that Caffey and Madell’s study remains the only large-scale systematic assessment of pubic ossification patterns in the general pediatric population; no contemporary study of comparable size has been published. Given current ethical considerations, comparable contemporary data are unlikely to become available, making this unique historical dataset the only available reference. Additionally, given the control data is from newborns while the patient group is in the 0–18 age range, the direct conclusion is methodologically problematic. The unusual ossification pattern of the pubic bone observed in children with SEDC formally demonstrated high specificity in our cohort both for the general population (based on published historical data) and in comparison with patients who had other COL2A1-related skeletal dysplasias. However, given the limitations of using historical control data, these specificity estimates should be interpreted cautiously. Consequently, the specificity values presented should be considered as preliminary estimates requiring validation in contemporary age-matched control populations.

5. Conclusions

We identified a rare phenomenon of atypical ossification of the superior ramus of the pubic bone, which may represent a supportive radiographic feature in the evaluation of patients with COL2A1-related skeletal dysplasias. This finding may be useful in the differential diagnosis of child abuse. Given the retrospective nature of this study and the limited size of non-SEDC subgroups, these findings should be validated in larger, prospective, age-matched cohorts. Further study of this condition may contribute to a better understanding of endochondral skeletal formation and the role of COL2A1 in this process.

Supplementary Materials

The following supporting information can be downloaded at: https://www.mdpi.com/article/10.3390/diagnostics16131955/s1, Table S1: Major diagnostic findings.

Author Contributions

Conceptualization and methodology, V.K. and T.M.; investigation and writing, V.K., T.M., E.M. and D.G. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

This study was carried out in accordance with the Code of Ethics of the World Medical Association (Declaration of Helsinki). The clinical and molecular genetic study was approved by the Institutional Review Board of the Research Centre for Medical Genetics, Moscow, Russia, (protocol code 2021-3) on 12 March 2021.

Informed Consent Statement

Informed consent was obtained from all subjects involved in the study.

Data Availability Statement

The data presented in this study are available on request from the corresponding author due to privacy.

Conflicts of Interest

The authors declare no conflicts of interest.

Abbreviations

The following abbreviations are used in this manuscript:
SEDCCongenital spondyloepiphyseal dysplasia
SEDSpondyloepiphyseal dysplasia
SEMDSpondyloepimetaphyseal dysplasia
COL2A1Collagen type II alpha 1 chain

References

  1. Unger, S.; Ferreira, C.R.; Mortier, G.R.; Ali, H.; Bertola, D.R.; Calder, A.; Cohn, D.H.; Cormier-Daire, V.; Girisha, K.M.; Hall, C.; et al. Nosology of genetic skeletal disorders: 2023 revision. Am. J. Med. Genet. Part A 2023, 191, 1164–1209. [Google Scholar] [CrossRef] [PubMed] [PubMed Central]
  2. Nenna, R.; Turchetti, A.; Mastrogiorgio, G.; Midulla, F. COL2A1 Gene Mutations: Mechanisms of Spondyloepiphyseal Dysplasia Congenita. Appl. Clin. Genet. 2019, 12, 235–238. [Google Scholar] [CrossRef] [PubMed] [PubMed Central]
  3. Anderson, I.J.; Goldberg, R.B.; Marion, R.W.; Upholt, W.B.; Tsipouras, P. Spondyloepiphyseal dysplasia congenita: Genetic linkage to type II collagen (COL2AI). Am. J. Hum. Genet. 1990, 46, 896–901. [Google Scholar] [PubMed]
  4. Spranger, J.W.; Brill, P.W.; Hall, C.; Nishimura, G.; Superti-Furga, A.; Unger, S. Bone Dysplasias: An Atlas of Genetic Disorders of Skeletal Development, 4th ed; Oxford University Press: Oxford, UK, 2018. [Google Scholar]
  5. Walter, K.; Tansek, M.; Tobias, E.S.; Ikegawa, S.; Coucke, P.; Hyland, J.; Mortier, G.; Iwaya, T.; Nishimura, G.; Superti-Furga, A.; et al. COL2A1-related skeletal dysplasias with predominant metaphyseal involvement. Am. J. Med. Genet. Part A 2007, 143A, 161–167. [Google Scholar] [CrossRef] [PubMed]
  6. Horton, W.A.; Hall, J.G.; Scott, C.I.; Pyeritz, R.E.; Rimoin, D.L. Growth curves for height for diastrophic dysplasia, spondyloepiphyseal dysplasia congenita, and pseudoachondroplasia. Am. J. Dis. Child. 1982, 136, 316–319. [Google Scholar] [CrossRef] [PubMed]
  7. Savarirayan, R.; Bompadre, V.; Bober, M.B.; Cho, T.J.; Goldberg, M.J.; Hoover-Fong, J.; Irving, M.; Kamps, S.E.; Mackenzie, W.G.; Raggio, C.; et al. Best practice guidelines regarding diagnosis and management of patients with type II collagen disorders. Genet. Med. 2019, 21, 2070–2080. [Google Scholar] [CrossRef] [PubMed]
  8. Gajarajulu, V.; Natarajan, B.; Muralinath, S. The Radiograph of the Pelvis as a Window to Skeletal Dysplasias. Indian J. Pediatr. 2016, 83, 543–552. [Google Scholar] [CrossRef] [PubMed]
  9. Jana, M.; Nair, N.; Gupta, A.K.; Kabra, M.; Gupta, N. Pelvic radiograph in skeletal dysplasias: An approach. Indian J. Radiol. Imaging 2017, 27, 187–199. [Google Scholar] [CrossRef] [PubMed]
  10. Terhal, P.A.; Nievelstein, R.J.; Verver, E.J.; Topsakal, V.; van Dommelen, P.; Hoornaert, K.; Le Merrer, M.; Zankl, A.; Simon, M.E.; Smithson, S.F.; et al. A study of the clinical and radiological features in a cohort of 93 patients with a COL2A1 mutation causing spondyloepiphyseal dysplasia congenita or a related phenotype. Am. J. Med. Genet. Part A 2015, 167, 461–475. [Google Scholar] [CrossRef] [PubMed]
  11. Asadulaev, M.S.; Vissarionov, S.V.; Pershina, P.A.; Malamashin, D.B.; Toria, V.G.; Kokushin, D.N.; Rybinskikh, T.S.; Belyanchikov, S.M.; Murashko, T.V. Surgical Correction of Kyphoscoliotic Spinal Deformity in a Child with Conradi–Hünermann Syndrome: A Case Report and Review. Pediatr. Traumatol. Orthop. Reconstr. Surg. 2025, 13, 307–318. [Google Scholar] [CrossRef]
  12. Matsushita, M.; Kitoh, H.; Kaneko, H.; Mishima, K.; Kadono, I.; Ishiguro, N.; Nishimura, G. A novel SOX9 H169Q mutation in a family with overlapping phenotype of mild campomelic dysplasia and small patella syndrome. Am. J. Med. Genet. Part A 2013, 161, 2528–2534. [Google Scholar] [CrossRef] [PubMed]
  13. Kleszczyński, J.; Błoch, M.; Hofbauer, K.; Dominiak, P. Metatropic dysplasia in four-year-old boy—Physiotherapy and orthopaedic care problemscase—Case report. Ortop. Traumatol. Rehabil. 2012, 14, 289–302, (In English and Polish). [Google Scholar] [CrossRef] [PubMed]
  14. Hosokawa, T.; Tanami, Y.; Sato, Y.; Oguma, E. Pubic bone ossification at birth in normal and preterm neonates. Pediatr. Int. 2022, 64, e15252. [Google Scholar] [CrossRef] [PubMed]
  15. Grissom, L.E.; Harty, M.P.; Guo, G.W.; Kecskemethy, H.H. Maturation of pelvic ossification centers on computed tomography in normal children. Pediatr. Radiol. 2018, 48, 1902–1914. [Google Scholar] [CrossRef] [PubMed]
  16. Caffey, J.; Madell, S.H. Ossification of the pubic bones at birth. Radiology 1956, 67, 346–350. [Google Scholar] [CrossRef] [PubMed]
  17. Perez-Rossello, J.M.; Connolly, S.A.; Newton, A.W.; Thomason, M.; Jenny, C.; Sugar, N.F.; Kleinman, P.K. Public ramus radiolucencies in infants: The good, the bad, and the indeterminate. AJR Am. J. Roentgenol. 2008, 190, 1481–1486. [Google Scholar] [CrossRef] [PubMed]
  18. Markova, T.; Kenis, V.; Melchenko, E.; Osipova, D.; Nagornova, T.; Orlova, A.; Zakharova, E.; Dadali, E.; Kutsev, S. Clinical and Genetic Characteristics of COL2A1-Associated Skeletal Dysplasias in 60 Russian Patients: Part I. Genes 2022, 13, 137. [Google Scholar] [CrossRef] [PubMed] [PubMed Central]
  19. Petrova, E.V.; Trofimova, S.I.; Agranovich, O.E.; Markova, T.V. Clinical and radiological variants of the nail–patella syndrome: Why is it important to make a correct diagnosis? Pediatr. Traumatol. Orthop. Reconstr. Surg. 2024, 12, 225–236. [Google Scholar] [CrossRef]
  20. Gorodilova, D.V.; Markova, T.V.; Kenis, V.M.; Melchenko, E.V.; Akinshina, A.D.; Ogorodova, N.Y.; Shchagina, O.A.; Dadali, E.L.; Kutsev, S.I. Clinical, genetic, and orthopedic characteristics of large group of patients with diastrophic dysplasia. Pediatr. Traumatol. Orthop. Reconstr. Surg. 2024, 12, 29–41. [Google Scholar] [CrossRef]
  21. VandenBerg, C.; Novais, E. Isolated congenital absence of inferior pubic rami ossification: A case report. J. Pediatr. Orthop. B 2014, 23, 541–543. [Google Scholar] [CrossRef] [PubMed]
  22. Mousafeiris, V.K.; Nikolopoulos, K.; Repantis, T. Pubic Bone Aplasia as an Incidental Finding in the Adult Population: Case Report and Review of the Literature. Cureus 2021, 13, e12703. [Google Scholar] [CrossRef] [PubMed] [PubMed Central]
  23. Wahlquist, M.; Iwinski, H.; Serey, P.J., Jr. Hypoplasia of the left superior ramus of the pubis. Am. J. Orthop. 2008, 37, 577–578. [Google Scholar] [PubMed]
  24. Verbruggen, S.W.; Nowlan, N.C. Ontogeny of the Human Pelvis. Anat. Rec. 2017, 300, 643–652. [Google Scholar] [CrossRef] [PubMed]
  25. Baumgart, M.; Wiśniewski, M.; Grzonkowska, M.; Badura, M.; Szpinda, M.; Pawlak-Osińska, K. Quantitative anatomy of the primary ossification center in the fetal pubis bone. Surg. Radiol. Anat. 2019, 41, 755–761. [Google Scholar] [CrossRef] [PubMed] [PubMed Central]
  26. Parvaresh, K.C.; Upasani, V.V.; Bomar, J.D.; Pennock, A.T. Secondary Ossification Center Appearance and Closure in the Pelvis and Proximal Femur. J. Pediatr. Orthop. 2018, 38, 418–423. [Google Scholar] [CrossRef] [PubMed]
  27. Okumura, M.; Ishikawa, A.; Aoyama, T.; Yamada, S.; Uwabe, C.; Imai, H.; Matsuda, T.; Yoneyama, A.; Takeda, T.; Takakuwa, T. Cartilage formation in the pelvic skeleton during the embryonic and early-fetal period. PLoS ONE 2017, 12, e0173852. [Google Scholar] [CrossRef] [PubMed] [PubMed Central]
  28. Parvaresh, K.C.; Pennock, A.T.; Bomar, J.D.; Wenger, D.R.; Upasani, V.V. Analysis of Acetabular Ossification from the Triradiate Cartilage and Secondary Centers. J. Pediatr. Orthop. 2018, 38, e145–e150. [Google Scholar] [CrossRef] [PubMed]
  29. Handa, A.; Grigelioniene, G.; Nishimura, G. Radiologic Features of Type II and Type XI Collagenopathies. RadioGraphics 2021, 41, 192–209. [Google Scholar] [CrossRef] [PubMed]
  30. Ablin, D.S.; Greenspan, A.; Reinhart, M.A. Pelvic injuries in child abuse. Pediatr. Radiol. 1992, 22, 454–457. [Google Scholar] [CrossRef] [PubMed]
  31. Kenis, V.M.; Baindurashvili, A.G.; Sapogovskiy, A.V.; Melchenko, E.V.; Kasev, A.N.; Shpulev, P.S. Musculoskeletal injuries and pain in children involved in sports: A literature review. Pediatr. Traumatol. Orthop. Reconstr. Surg. 2024, 12, 271–283. [Google Scholar] [CrossRef]
Table 1. Frequency of multiple ossification centers of the superior pubic ramus in different COL2A1-related phenotypes and in the general population (historical data from Caffey & Madell, 1956 [16]).
Table 1. Frequency of multiple ossification centers of the superior pubic ramus in different COL2A1-related phenotypes and in the general population (historical data from Caffey & Madell, 1956 [16]).
SEDCKniest DysplasiaStickler SyndromeSEDGeneral Population (Caffey and Madell, 1956 [16])
Total551232301286
Multiple ossification centers2000019
One ossification center311232301266
No ossification40001
Table 2. Ossification patterns of the superior pubic ramus in SEDC patients by age group.
Table 2. Ossification patterns of the superior pubic ramus in SEDC patients by age group.
Age
OssificationUp to 1 Year1–10 Years>10 Years
Multiple ossification centers10100
One ossification center8147
No ossification400
Total24247
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content.

Share and Cite

MDPI and ACS Style

Kenis, V.; Markova, T.; Melchenko, E.; Gorodilova, D. Multiple Ossification Centers of the Pubic Bone as a Supportive Radiographic Feature for COL2A1-Related Congenital Spondyloepiphyseal Dysplasia. Diagnostics 2026, 16, 1955. https://doi.org/10.3390/diagnostics16131955

AMA Style

Kenis V, Markova T, Melchenko E, Gorodilova D. Multiple Ossification Centers of the Pubic Bone as a Supportive Radiographic Feature for COL2A1-Related Congenital Spondyloepiphyseal Dysplasia. Diagnostics. 2026; 16(13):1955. https://doi.org/10.3390/diagnostics16131955

Chicago/Turabian Style

Kenis, Vladimir, Tatiana Markova, Evgeniy Melchenko, and Daria Gorodilova. 2026. "Multiple Ossification Centers of the Pubic Bone as a Supportive Radiographic Feature for COL2A1-Related Congenital Spondyloepiphyseal Dysplasia" Diagnostics 16, no. 13: 1955. https://doi.org/10.3390/diagnostics16131955

APA Style

Kenis, V., Markova, T., Melchenko, E., & Gorodilova, D. (2026). Multiple Ossification Centers of the Pubic Bone as a Supportive Radiographic Feature for COL2A1-Related Congenital Spondyloepiphyseal Dysplasia. Diagnostics, 16(13), 1955. https://doi.org/10.3390/diagnostics16131955

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop