Imaging & Diagnostics

Knee Complaints: Diagnostic Imaging Approach & Neoplasms

Bone Neoplasms Tumor-Like Conditions

  • Bone neoplasms and tumor-like conditions affecting the knee can be benign or malignant. Age at Dx is crucial for DDx
  • In patients <40: Benign bone neoplasms: Osteochondroma, Enchondroma are relatively frequent
  • Fibrous cortical defect (FCD) & Non-ossifying fibroma (NOF) are particularly frequent in children
  • Giant cell tumor (GCT) is the m/c benign neoplasm of the knee in patients between 20-40 years of age
  • Malignant bone neoplasms in <40: m/c Osteosarcoma and 2nd m/c Ewing sarcoma
  • In patients >40: malignant neoplasms: m/c are secondaries d/t bone metastasis. Primary bone malignancy: the m/c
  • Multiple Myeloma (MM). Less frequently: 2nd peak of Osteosarcoma (post-radiation or Paget’s), Fibrosarcoma or Malignant Fibrous Histeocytoma (MFH) of bone.
  • Clinically: knee pain, pathological fracture
  • Some tumor-like conditions like FCD/Non-ossifying fibroma are asymptomatic and may regress spontaneously. 
    Occasionally NOF may present with pathologic fracture. N.B. any knee/bone pain in a child/adolescents should be treated with clinical suspicion and properly investigated.
  • Imaging: 1st step: radiography
  • MRI with T1+C is crucial for lesion characterization/regional extent, staging and pre-operative planning. CT may help with pathologic Fxs detection. If malignant bone neoplasms considered, CXR/CT, PET-CT to investigate metastatic spread and staging are important

Imaging Approach Bone Neoplasms

  • Approach to imaging Dx of bone neoplasms includes: age, bone location (epiphysis vs metaphysis vs diaphysis), zone of transition surrounding the lesion, periosteal response, type of matrix, permeating or moth-eaten destruction vs. sclerotic, ground-glass, osteoid, cartilaginous matrix, soft tissue invasion etc.
  • Key x-radiography features to DDx benign vs malignant bone neoplasm:
  • Zone of transition: lesion is geographic with narrow zone of transition vs ill-defined wide zone of transition suggesting aggressive bone resorption
  • What type of bone destruction occurred: soap-bubbly appearance vs. osteolytic vs. osteosclerotic changes
  • Is there a round-glass matrix? Is there a well-defined rim of sclerotic border with septations potentially suggesting slow growth and encapsulation like most benign processes.
  • Periosteal proliferation: solid vs. aggressive spiculated/sunburst/hair-on-end with local soft tissue invasion and Codman triangle (study next slide)

FCD & NOF

  • FCD & NOF or more appropriately Fibroxanthoma of the bone are benign bone processes that m/c seen in children. DDx based on the size with FCD presenting as <3-cm and NOF >3cm lesion composed of fibrous heterogeneous matrix. FCD are asymptomatic and may regress in many cases. Some may progress to NOF. Location: identified in the knee region as eccentric cortical based lesion.
  • FCD must be DDx from an avulsive irregularity d/t repeated stress along Linea aspera by extensors muscles
  • Dx: radiography
  • Management: leave-me-alone lesion. Occasionally NOF may progress and lead to pathologic fracture requiring orthopedic consult

Osteochondroma

  • Osteochondroma: m/c benign bone neoplasm. Knee is the m/c location. Contains all bone elements with cartilaginous cap. Presented as pedunculated or sessile bone exostosis pointing away from the joint.
  • 1% malignant degeneration to chondrosarcoma if solitary lesion and 10-15% in cases of HME
  • Other complications: fracture (top left image) pseudoaneurysm of Popliteal artery, adventitious bursa formation
  • Hereditary Multiple Exostosis (HME)– autosomal dominant process. Presents with multiple osteochondromas (sessile-type dominates). May lead to limb deformities (Madelung deformity, coxa valga) reactive ST pressure, malignant degeneration
  • Dx: radiography, MRI helps to Dx malignant degeneration to chondrosarcoma by changes in size and activity of cartilaginous cap (>2-cm in adults may manifest malignant degeneration). MRI will also help with Dx of regional complications

HME & Knee Pain

37-y.o male with HME and knee pain. Axial T1, T2 and STIR MRI slices at popliteal region. Large cartilaginous cap and possible compression of the popliteal artery by osteochondroma. MRA was performed to evaluate popliteal A. pseudoaneurysm (large arrow). Pathology specimen obtained from the cartilagenous cap showed increased cellularity suggestive of malignant degeneration. Operative care was planned

Giant Cell Tumor (GCT) aka Osteoclastoma

  • GCT- is a relatively common primary benign bone neoplasm. Age 25-40. M>F slightly.
  • M/C location: Distal femur>proximal tibia>distal radius>sacrum
  • GCT is the M/C benign sacral tumor. In 50% cases GCT occurs about the knee.
  • GCT is histologically benign but lung mets may develop esp. if in distal radius and hands, often termed Malignant GCT
  • <1% unresponsive/recurring GCTs may undergo malignant transformation to high grade bone sarcoma
  • Pathology: histologically composed of osteoclasts-multinucleated giant cells with stromal cells derived from precursors monocytemacrophage type. Produces cytokines and osteolytic enzymes. GCT may contain blood and associated with secondary Aneurysmal Bone Cyst (ABC)
  • Clinically: knee pain unresponsive to conservative care. Pathologic Fx may occur
  • Imaging: always begins with radiography followed by MRI and surgical biopsy that are crucial to Dx.
  • Rx: operative with curettage and cementing, surgical appliance may be used if pathological fx present and cortical breach. In more severe cases other options available

Radiologic Pathologic Dx

  • Radiologic-pathologic Dx: osteolytic and/or soap-bubbly lesion typically involving metaphysis and into epiphysis (classic key feature) with subarticular extension. Zone of transition is typically narrow but occasionally in aggressive lesions wide zone of transition may be seen.
  • MRI: low T1, highT2/STIR, characteristic fluid-fluid levels noted that are present in GCT and ABC. Histology is crucial to Dx.
  • DDx: ABC, Brown cell tumor of HPT (osteoclastoma), Telangectatic Osteosarcoma
  • Radiological rule: if physeal growth plate is present Dx of GCT is taken off the list in favour of chondroblastoma and vice versa.

Primarily Soap-Bubbly Appearance of GCT

Coronal, Fat-Sat Sagittal & Axial MRI Slices of GCT

  • T1 coronal, T2 fat-sat sagittal and T2 axial MRI slices of GCT. Typically: low T1, highT2/STIR and fluid-fluid levels

Characteristic MRI Appearance of GCT

  • Fluid-fluid levels d/t different composition of blood degradation products
  • Important DDx: ABC

Malignant Neoplasms About the Knee

  • In children and very young adults m/c primary malignant neoplasm is central aka intramedullary (osteogenic) osteosarcoma (OSA). Second peak of OS: >70 y.o d/t Paget’s (1%) and/or postradiation OSA.
  • Knee is the m/c location of OSA (distal femur, prox. Tibia)
  • 2nd m/c malignant pediatric primary is Ewing sarcoma.
  • In adults >40 y.o. the m/c primary is Multiple Myeloma (MM) or Solitary Plasmacytoma
  • Overall m/c bone neoplasms in adults d/t bone mets from lung, breast, prostate, renal cell, thyroid (discussed)
  • Dx: clinical and radiological with surgical biopsy
  • Imaging is crucial to Dx. 1st step x-radiography. MRI+ gad C is crucial
  • CT scanning occasionally helps to evaluate pathological fracture

Central (Intramedullary) Osteosarcoma (OSA)

  • m/c age: 10-20. m/c location: knee, males>females. Increased risk in some
  • congenital syndromes and mutation of the retinoblastoma gene: Rothmund-Thompson AR syndrome.
  • Early Dx is important d/t 10-20% present with Lung mets at Dx. Prognosis depends on stages. Early stages with local bone invasion and no
  • mets 76% of survival.
  • Rx: limb salvage procedures preferred with 8-12 weeks of chemo, amputation if encased neurovascular tissue, path Fx etc.
  • Imaging: radiography and MRI.
  • Clinically: bone pain, inc. Alkaline Phosphatase
  • Chest CT if lung mets considered

Classic Rad Features of OSA

  • Osteoid forming sclerotic mass with aggressive hair-on-end/speculated/sun-burst periosteal reaction, Codman’s trangle and soft tissue invasion. Order MRI for staging and extent. Chest CT is crucial for Lung Mets dx.

MRI is Crucial for Dx/Staging

  • Note: sagittal T1 (left) and STIR (right) MR slices: large mass extending from distal femoral metaphysis to remaining shaft. Low signal on T1 and high on STIR d/t marrow invasion with edema,hemorrhaging and tumor invasion. Local ST invasion seen (white arrows). Periosteal lifting and Codman’s triangle (green arrow) are additional signs of aggressive neoplasm.
  • Note an interesting feature that the epiphysis is spared d/t physeal plate serving temporarily as an additional barrier to the tumour spread.

Ewing Sarcoma

Ewing sarcoma: age: 2-20, uncommon in black patients. 2nd m/c highly malignant bone neoplasm in children that typically arises from
medullary cavity (Round cell tumors). Key symptom: bone pain that may mimic infection (ESR/CRP/WBC) Considered PNET
Key Rad Dx: aggressive moth-eaten/permeative lucent lesions in the shaft of long bones with large soft tissue invasion/typical onion skin
periostitis. May produce saucerisation
May affect flat bones. May appear as sclerotic in 33%. Early lung mets (25-30%) bone-to-bone mets
Poor prognosis if delayed Dx. Imaging steps: 1st step x-rad, MRI is v. important followed by biopsy. CXR/CT PET-CT
Rx: combined rad-chemo, operative.

M/C Malignant Knee Neoplasms in Adults

  • 66-y.o. male with knee pain
  • Note aggressive expansile osteolytic lesion in the distal femur metaphysis into epiphysis. No periosteal reaction present. Following further work up with abdominal and chest CT scanning, Dx of Renal cell carcinoma was established
  • Distal mets into lower extremity are more common with lung, renal cell, thyroid and breast CA.
  • Renal cell and Thyroid will typically present with aggressive osteolytic expansile mass aka “blowout mets”
  • In general, imaging approach should consist of Radiographic knee series, followed by MRI if xrays are unrewarding
  • Tc99 Bone scintigraphy is the modality of choice to evaluate metastatic bone disease

Soft Tissue Neoplasms About the Knee

Malignant fibrous histiocytoma (MFH) reclassified as Pleomorphic Undifferentiated Sarcoma (PUS) is the m/c S.T. sarcoma. MFH is
aggressive biologically with poor prognosis
M>F (1.2:1) 30-80 with peak in a 6th decade. 25-40% of all adults sarcomas m/c extremities. Retroperitoneum next (worst prognosis d/t late Dx and large growth w/o symptoms)
Clinically: painful, hard mass typically about the knee or thigh. Histology: poorly differentiated/undifferentiated malignant fibroblasts, myofibroblasts and other mesenchymal cells
Imaging: MRI is the modality of choice with T1, T2, T1+C. Typically appears as aggressive heterogeneous mass intermediate to low signal on T1 and high signal on T2 with areas of necrosis and enhancement on T1+C. May
appear misleadingly encapsulated w/o true capsule
Management: operative with radiation and chemotherapy. Tumour depth is crucial for prognosis. 80% 5-year survival if <5cm deep in ST and 50% if >5-cm deep in ST.

Synovial Sarcoma

Synovial sarcoma: common malignant ST neoplasm esp. in younger patients or older children/adolescents. M/C found in knee area
Clinically: can present slowly as palpable mass in the extremity often ignored d/t slow growth
Imaging is the key: radiography may reveal ST. density/mass. Some synovial sarcomas may show calcification and mistaken for Myositis Ossificanse or heterotopic bone formation
MRI with T1,T2 and T1+C are Dx modality of choice. Other modalities: US, CT are non-specific
DDx: MFH
Management: operative, chemo-radiation
Prognosis: variable depending on size, invasion, metastasis

For Complete List Of Bone & Soft Tissue Neoplasms

Neoplasms of the Knee

Post Disclaimer

Professional Scope of Practice *

The information herein on "Knee Complaints: Diagnostic Imaging Approach & Neoplasms" is not intended to replace a one-on-one relationship with a qualified health care professional or licensed physician and is not medical advice. We encourage you to make healthcare decisions based on your research and partnership with a qualified healthcare professional.

Blog Information & Scope Discussions

Our information scope is limited to Chiropractic, musculoskeletal, physical medicines, wellness, contributing etiological viscerosomatic disturbances within clinical presentations, associated somatovisceral reflex clinical dynamics, subluxation complexes, sensitive health issues, and/or functional medicine articles, topics, and discussions.

We provide and present clinical collaboration with specialists from various disciplines. Each specialist is governed by their professional scope of practice and their jurisdiction of licensure. We use functional health & wellness protocols to treat and support care for the injuries or disorders of the musculoskeletal system.

Our videos, posts, topics, subjects, and insights cover clinical matters, issues, and topics that relate to and directly or indirectly support our clinical scope of practice.*

Our office has reasonably attempted to provide supportive citations and has identified the relevant research study or studies supporting our posts. We provide copies of supporting research studies available to regulatory boards and the public upon request.

We understand that we cover matters that require an additional explanation of how it may assist in a particular care plan or treatment protocol; therefore, to further discuss the subject matter above, please feel free to ask Dr. Alex Jimenez, DC, or contact us at 915-850-0900.

We are here to help you and your family.

Blessings

Dr. Alex Jimenez DC, MSACP, RN*, CCST, IFMCP*, CIFM*, ATN*

email: coach@elpasofunctionalmedicine.com

Licensed as a Doctor of Chiropractic (DC) in Texas & New Mexico*
Texas DC License # TX5807, New Mexico DC License # NM-DC2182

Licensed as a Registered Nurse (RN*) in Florida
Florida License RN License # RN9617241 (Control No. 3558029)
Compact Status: Multi-State License: Authorized to Practice in 40 States*

Presently Matriculated: ICHS: MSN* FNP (Family Nurse Practitioner Program)

Dr. Alex Jimenez DC, MSACP, RN* CIFM*, IFMCP*, ATN*, CCST
My Digital Business Card

Dr. Alex Jimenez

Specialties: Stopping the PAIN! We Specialize in Treating Severe Sciatica, Neck-Back Pain, Whiplash, Headaches, Knee Injuries, Sports Injuries, Dizziness, Poor Sleep, Arthritis. We use advanced proven therapies focused on optimal mobility, posture control, health Instruction, functional fitness, and structural conditioning. In addition, we use effective "Patient Focused Diet Plans," Specialized Chiropractic Techniques, Mobility-Agility Training, Cross-Fit Protocols, and the Premier "PUSH Functional Fitness System" to treat patients suffering from various injuries and health problems. Ultimately, I am here to serve my patients and community as a Chiropractor, passionately restoring functional life and facilitating living through increased mobility.

Published by

Recent Posts

Massage Gun Use: Relaxation and Pain Relief for Expecting Moms

Stress on the lower back during pregnancy often leads to back (upper, middle, lower), sciatica,… Read More

December 20, 2024

Melatonin: How it Can Help Improve Sleep Quality

Can melatonin help many individuals dealing with sleep issues and help them stay asleep longer… Read More

December 20, 2024

Stay Fit and Strong at Any Age with Kettlebell Training

For older individuals looking for a workout that can help improve overall fitness, can kettlebell… Read More

December 19, 2024

Say Goodbye to Neck Pain: Find the Ideal Pillow for You

Can choosing the right pillow help many individuals with neck pain get a full night's… Read More

December 19, 2024

Achieve Pain-Free Sleep with the Right Mattress for Back Pain

What is the recommended way to choose a mattress for individuals with back pain?  … Read More

December 18, 2024

Piriformis Syndrome: Exploring Non-Surgical Treatment Methods

Can non-surgical treatments help individuals with piriformis syndrome reduce referred sciatica pain and help restore… Read More

December 18, 2024