Orthopedic Pathology

Question 1

What what are the epiphysis and metaphysis called in immature skeletons?

Answer 1

epiphyseal growth plate or “physis”

growth plate cartilage is replaced by bone in skeletally mature individuals

Question 2

periosteum

Answer 2

specialized connective fibrous tissue with osteogenic potential

covers bone but is absent in joint spaces at attachment sites of tendons or ligaments

Question 3

endosteum

Answer 3

inner lining of diaphyis and of cancellous bone

also has osteogenic potential

Question 4

intramembranous bone

Answer 4

arises from collagen

forms flat bones of skull and clavicles and responsible for prepubertal bone widening

Question 5

enchondral bone

Answer 5

arises from epiphyseal cartilage (growth plate)

forms appendicular and axial skeleton and responsible for prepubertal bone lengthening

Question 6

What are the zones of echondral bone formation, starting from the tip?

Answer 6

resting zone

zone of proliferation

zone of hypertrophy

zone of provisional calcification

primary trabeculae

Question 7

resting zone

Answer 7

inactive chondrocytes

Question 8

zone of proliferation

Answer 8

chondrocytes proliferate and begin to secrete cartilaginous matrix

Question 9

zone of hypertrophy

Answer 9

chondrocytes enlarge, form columns, and secrete cartilaginous matrix

Question 10

zone of provisional calcification

Answer 10

vitamin D causes matrix calcification and entrapped chondrocytes undergo apoptosis

Question 11

primary trabeculae

Answer 11

scaffolds of dead cartilage form the framework on which osteoprogenitor cells (transported through newly formed vessels in the growth plate) deposit bone matrix

Question 12

What diseases arise from defects in the zone of proliferation?

Answer 12

thanataphoric/achondroplastic dwarfism

mucopolysaccharidosis

Question 13

What diseases arise from defects in the zone of provisional calcification?

Answer 13

Ricets/Osteomalacia

Question 14

What diseases arise from defects in the primary trabeculae?

Answer 14

osteogenesis imperfecta/scurvy/osteopetrosis

Question 15

What are the types of bone?

Answer 15

immature - osteoid and woven bone

mature - lamellar bone

Question 16

osteoid bone

Answer 16

unmineralized, poorly organized immature bone matrix (Type I collagen) formed rapidly (long arrow)

ex. new bone covering lamellar/woven bone (10% of normal bone is covered by osteoid), tumor bone, rickets (osteomalacic) bone

Question 17

woven bone

Answer 17

mineralized immature bone formed rapidly (short arrow)

high number of active osteoblasts

ex. fracture callus, sites of bone repair, periosteal reaction to infection or neoplasia

Question 18

lamellar bone

Answer 18

mineralized mature bone formed slowly

parallel collagen type I fiber sheets/bundles (lamellae), evenly distributed osteocytes

two types - cortical (compact) bone and cancellous (spongy) bone

Question 19

cortical (compact) bone

Answer 19

85% of lamellar bone

collagen type I first deposited in the circumferential lamellae

concentric lamellae later develop osteons that dissipate mechanical stress

Question 20

cancellous (spongy) bone

Answer 20

15% of lamellar bone

lamella collagen type I aligned longitudinally in response to mechanical stress

formed by enchondral ossification and constantly remodeled to dissipate stress

Question 21

osteoblasts

Answer 21

derived from mesenchymal stem cells and line surface of bone

cell surface receptors include PTH, vitamin D, estrogen, insulin-like growth factor-1 (somatomedin), and others

produce matrix proteins and type I collagen, and initiate mineralization

Question 22

osteocytes

Answer 22

osteoblasts that are incorporated into mature bone (most common cells within bone)

cell processes communicate through canaliculi within osteon unit

important in regulating calcium and phosphate

mechanical forces cause transcriptional activation of cAMP pathways within osteocytes resulting in remodeling of bone (mechanotransduction)

produce sclerostin - protein that inhibits bone formation

Question 23

osteoclasts

Answer 23

multinucleated cells formed from monocytic progenitor cells in response to RANK-ligand secreted from osteoblasts and bone stromal cells

responsible for bone resorption

located in “resorption pits” or Howship’s lacunae

Question 24

What are the functions of osteoclasts that bind in the Howship lacunae?

Answer 24

acidify etracellular space resulting in release of minerals into serum and secrete digestive enzymes (cathepsisns) that dissolve organic matrix resulting in bone resorption

release growth factors and cytokines incorporated in bone that stimulate proliferation of osteoblasts

this interaction between osteoclasts and osteoblasts insures normal physiologic bone remodeling throughout life in response to mechanical stress

Question 25

osteoclast “resorption pit”

Answer 25

forms a sealed acidified microenvironment in “resorption pits” on the surface of the bone

“ruffled” membrane contains H+ ATPase

HCl mobilizes the mineral phase and proteinase cathepsin K degrades the organic matrix

these actions release minerals and growth factors from bone

Question 26

What is the process of bone remodeling in cancellous bone?

Answer 26

activation of osteoclasts

resorption of bone in Howship’s lacuna

“reversal” of cell type with osteoblasts

bone formation

Question 27

What is the process of osteon formation in cortical bone?

Answer 27

osteons form in response to stress

first osteoclastic resorption (“cutting cones”)

osteon then filled with bone produced by osteoblasts in a concentric fashion

osteocytes (most common cellular element) within rings of the osteon communicate through dendritic processes and regulate bone remodeling and mineral stores

Question 28

What are the primary causes of acute osteomyelitis?

Answer 28

primarily caused by bacterial infection resulting from:

1) hematogenous spread
2) contiguous spread from adjacent extra-osseous site
3) direct inoculation of organism into bone
4) ischemia (vascular insufficiency)

**Staphyloccocus aureus is the most common

infection localizes in the vascularized regions of bone, can seed periosteal tissue through the Volkman canals

Question 29

What are the histological features of acute osteomyelitis?

Answer 29

microscopically, acute inflammatory cells are ultimately associated with non-viable bone (sequestrum)

periosteum/endosteum responds by forming new bone (involucrum) around the dead, infected bone

managed by surgery and a long course of antibiotics

Question 30

categories of bone diseases

Answer 30

abnormal matrix

too little matrix

too little mineralization

too much bone resorption

too little bone resorption

Question 31

What are the types of osteogenesis imperfecta? What is the cause?

Answer 31

four distinct phenotypic and genetic groups

autosomal recessive form is most severe and lethal in perinatal period

caused by defect in syhtnesis of Type I collagen - abnormal type I collagen results in more serious disease than decreased synthesis of collagen

Question 32

What are the physical outcomes of osteogenesis imperfect?

Answer 32

affects bone (fractures that resolve with excess callus formation)

dentin of teeth (dentinogenesis imperfecta)

eyes (thin sclera allow visualization of choroidal vasculature resulting in blue sclera)

ligaments (joint laxity and early osteoarthritis)

and ossicles of the ear (hearing defects).

Question 33

What are the histological features of osteogenesis imperfecta?

Answer 33

cartilaginous columns are not converted to bone

medullary cavity containing thin trabecular bone and marrow fibrosis

Question 34

osteoporosis

Answer 34

Definition: Bone that is histologically normal but decreased in quantity. Clinically defined as ≥ 1 atraumatic fractures or low bone mineral density on bone density scan (dual-energy x-ray absorptiometry). Process can be-

1. ) Localized-immobility (Sudeck’s atrophy), inflammation
2. ) Generalized -Senile & postmenopausal osteoporosis are the two most common forms of the disorder. Osteoporosis also occurs with endocrinopathies, type 1 diabetes mellitus, scurvy, OI, drugs (corticosteroids), ¯Vitamin D, and space travel.

Question 35

pathogenesis of senile and postmenapausal osteoporosis

Answer 35

Depends upon initial bone density and subsequent loss of bone that occurs with age

Bone mass peaks in early adulthood (75% dependent on genetics & 25% function of environment)

With aging, osteoblasts lose their ability to form new bone and growth factors lose potency

Bone loss is further accentuated by activation of osteoclasts

Question 36

postmenopausal osteoporosis

Answer 36

after menopause, estrogen deficiency up-regulates osteoclastogenic factors IL-1, IL-6, & TNF-a and decreases OPG resulting in osteoclastogenesis

up to 2% cortical and 9% cancellous bone lost per year

affects bones with large surface area (ie., vertebral body) (right). Fractures of vertebra and wrist

high-turnover osteoporosis-activity of osteoclasts>osteoblasts

Question 37

senile osteoporosis

Answer 37

men and women > 80 years of age

caused by:

1) osteoblasts have decreased reproductive and biosynthetic potential with age
2) growth factors in matrix less potent

thin cortex leads to fractures involve hip and vertebra

low-turnover osteoporosis (decreased activity of osteoblasts, normally active osteoclasts)

Question 38

vitamin D deficiency (RIckets/Osteomalacia)

Answer 38

Increased PTH (due to decreased serum calcium) and decreased serum phosphate stimulate Vitamin D synthesis by 1-hydroxylation of 25-hydroxycholecalciferol in kidney

Vitamin D, in turn, suppresses PTH gene expression and PTH secretion from parathyroid gland

Hypovitaminosis D is presently considered a pandemic problem. 25% of elderly individuals suffer mild osteomalacia due to lack of sun exposure and ↓ calcium and magnesium intake.

Question 39

What are the results of vitamin D deficiency?

Answer 39

inability to calcify the zone of hypertrophy in developing growth plate (so chondrocytes do not die and are not replaced by bone)

inability to calcify osteoid formed throughout life during remodeling process

Question 40

What is the role of vitamin D?

Answer 40

Vitamin D increases calcium and phosphate absorption from the intestine

During enchondral bone formation, it is required for the calcification of cartilaginous matrix that surrounds chondrocytes in the Zone of Provisional Calcification of the growth plate (rickets)

In adults, required for calcification of osteoid (osteomalacia)

Question 41

pathological findings in Rickets (osteomalacia)

Answer 41

In children (Vitamin D deficiency), growth plate becomes widened with cartilage (“metaphyseal flare”)

Cartilage matrix (star) and newly formed osteoid (right lower) do not calcify. (normal growth plate on left)

Question 42

What are the important features of osteomalacia?

Answer 42

osteomalacia in adults is usually due to chronic renal failure (renal osteodystrophy) caused by-

1) Decreased serum calcium, phosphate retention and decreased synthesis of Vitamin D (due to loss of kidney mass).
2) Decreased serum calcium leads to increased PTH (“secondary” hyperparathyroidism)

Osteomalacia results in long bone ”insufficiency” fractures on Xray and bone pain.

Question 43

What are the histological features of osteomalacia?

Answer 43

Osteomalacia in adults is usually due to chronic renal failure (renal osteodystrophy)

osteomalacic bone shows excess osteoid (LEFT, calcium stains black; RIGHT, trichrome stain with red osteoid).

Question 44

What are the clinical findings of hyperparathyroidism?

Answer 44

(GI tract) moans, bones,(renal) stones, and psychiatric overtones

Question 45

What is the pathogenesis of hyperparathyroidism?

Answer 45

primary (most commonly, adenoma and less often, primary chief cell hyperplasia) and secondary causes (most often in response to chronic renal failure)

increased PTH results in osteoclastogenesis

affects cortical > cancellous bone (bone loss in fingers & clavicles by Xray)

Question 46

What are the histological findings of hyperparathyroidism

Answer 46

microscopically, aggregates of activated osteoclasts form “cutting cones” that resorb bone

“dissecting osteitis” - railroad track appearance of bony trabeculi due to central resorption by osteoclasts (leads to loss of bone-osteoporosis)

subperiosteal cortical bone resorption by osteoclasts

severe disease (most often occurring in secondary hyperparathyroidism) causes fractures that result in hemorrhage, cyst formation,& fibrosis (“osteitis fibrosa cystica” or “brown tumor of bone”)

enlarged Haversian canals

Question 47

dissecting osteitis

Answer 47

result of hyperparathyroidism

aggregates of activated osteoclasts form a “cutting cone” along the longitudinal axis of a trabecula

Question 48

brown tumor of bone “osteitis fibrosa cystica”

Answer 48

spindled stromal cells, osteoclasts, foci of hemorrhage, and hemosiderin deposits (arrow)

Question 49

What is the definition of Paget’s disease of bone

Answer 49

“Collage of matrix madness” due to dyssynchrony of osteoclastic/osteoblastic activity Older population; European Caucasians

Question 50

What are the types of Paget’s disease of bone, and what are the phenotypic manifestations?

Answer 50

Polyostotic (85%) > monostotic (15%)

femur or axial skeleton involved in 80% of cases

Results in “chalk stick” fractures, cranial/spinal nerve deficits, high-output cardiac failure (↑ marrow vascularity), & rarely, sarcomatous transformation (mostly, craniofacial and axial bones)

Question 51

What are the three phases of Paget’s disease of bone?

Answer 51

Marked bone resorption followed by rapid new bone formation:

1) osteolytic - numerous, enlarged osteoclasts >100 nuclei per cell and highly vascular marrow
2) “mixed” osteoblastic/osteolytic
3) sclerotic - thickened bone exhibiting a haphazard arrangement of cement lines

Question 52

What are the histologic findings of Paget’s disease of bone?

Answer 52

abnormally large osteoclasts with >100 nuclei per cell, thickened bone with hapazard cement lines

Question 53

What is the pathogenesis of Paget’s disease of bone?

Answer 53

Pathogenesis involves viral and genetic interactions: Mutated p62, a key regulator of RANKL/NFKB

mediated osteoclastogenesis, sensitizes osteoclast precursors to RANKL, while paramyxovirus stimulates osteoclastogenesis resulting in an increased number of multinucleated osteoclasts with enhanced resorption capacity

Question 54

What are the radiographic and histologic findings of Paget’s Disease?

Answer 54

radiograph shows characteristic tapering lytic process in the distal femur (top,left)

highly vascularized stroma occasionally results in high-output cardiac failure (top, right)

enlarged osteoclasts active during the early osteolytic phase of the disease (bottom, left; arrows)

osteosclerotic phase of disease is characterized by thickened bone with a haphazard (mosaic) pattern of cement lines (bottom, right)

Question 55

What are the characteristics of osteopetrosis?

Answer 55

absent or defective osteoclast activity (in most cases, osteoclasts fail to acidify “resorption” pits)

failure of bone remodeling resulting in abnormally thickened bone

Question 56

What are the clinical features of osteopetrosis?

Answer 56

fractures (no osteon formation)

anemia/thrombocytopenia/infections

deforming extramedullary hematopoiesis

cranial nerve defects