Osteoporosis resident survival guide
For Osteoporosis click here.
Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Eiman Ghaffarpasand, M.D. [2]
| Osteoporosis Resident Survival Guide Microchapters |
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| Overview |
| Classification |
| Causes |
| FIRE |
| Diagnosis |
| Treatment |
| Do's |
| Don'ts |
Overview
Osteoporosis was first discovered by John Hunter, British surgeon, in 1800's. Osteoporosis divided to primary and secondary diseases, upon classification based on disease origin. While, it becomes divided to osteopenia, osteoporosis, and severe osteoporosis, upon classification based on disease severity. The pathophysiology of osteoporosis basically involves an imbalance between bone resorption and bone formation. Major factors that contribute to the development of osteoporosis include estrogen deficit and aging. The main pathway, through which these factors might lead to osteoporosis is reactive oxygen species (ROS) damage to osteocytes. Decreasing the capability of autophagy in osteocytes is another important issue; which make them vulnerable to oxidative stresses. Genes involved in the pathogenesis of osteoporosis are many genes that majorly can categorized in four main groups, include the osteoblast regulatory genes, osteoclast regulatory genes, bone matrix elements genes, and hormone/receptor genes. Osteoporosis must be differentiated from other diseases that cause decreasing in bone mineral density (BMD), such as idiopathic transient osteoporosis of hip, osteomalacia, scurvy, osteogenesis imperfecta, multiple myeloma, homocystinuria, and hypermetabolic resorptive osteoporosis. Osteoporosis is a major health problem involving 43.9% (43.4 million) of male and female population in the United States. White females and African-American males have the highest frequency among the other races. Risk factors for osteoporosis disease are of two types, including non-modifiable and modifiable (potentially) factors. Non-modifiable risk factors are age, sex, menopause, and family history. Modifiable (potentially) factors are smoking, alcohol consumption, immobility, glucocorticoid abuse, and proton pump inhibitor (PPI). Today, risk of fracture due to osteoporosis is threatening one out of two postmenopausal women and also one out of five older men. The 10-year risk for any osteoporosis-related fractures in 65-year-old white woman with no other risk factor is 9.3%. Upon the guidelines of USPSTF, all women ≥ 65 years old along with women < 65 years old with high risk of fracture are target of screening for osteoporosis; but there is not any recommendation to screen men for the disease. There are two major methods, that is suggested to use for screening osteoporosis, include dual energy x-ray absorptiometry (DXA) of both hip and lumbar spine bones, and quantitative ultrasonography of the calcaneus. If left untreated, most of patients with osteoporosis may progress to develop fracture. With appropriate and timely usage of medications along with calcium and/or vitamin D supplementation, the outcome of osteoporosis is usually good. The mainstays of treatment in primary osteoporosis disease are based on in lifestyle modifications. Most of the time in high risk patients and people with past history of osteoporotic fracture, medical therapy is necessary. Bisphosphonates are the first line treatment for osteoporosis disease. Raloxifene is the second line treatment of osteoporosis in postmenopausal women, for both treatment and prevention. Denosumab is a human monoclonal antibody designed to inhibit RANKL (RANK ligand), a protein that acts as the primary signal for bone removal. It is used to treat Osteoporosis in elder men and postmenopausal women. Teriparatide and Abaloparatide are human recombinant parathyroid hormones used to treat postmenopausal woman with osteoporosis at high risk of fracture or to increase bone mass in men with osteoporosis.
Classification
Osteoporosis may be classified into several subtypes based on disease origin, and disease severity.
| Osteoporosis classifications | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
| Based on Disease severity | Based on Disease etiology | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
| T-score measurement | Bone loss due to other diseases? | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
| -1>T-score>-2.5 | T-score≤-2.5 | T-score≤-2.5 plus history of fracture | No | Yes | |||||||||||||||||||||||||||||||||||||||||||||||||||||||
| Osteopenia | Osteoporosis | Severe osteoporosis | Primary osteoporosis | Secondary osteoporosis | |||||||||||||||||||||||||||||||||||||||||||||||||||||||
Juvenile Osteoporosis (JO)
Osteoporosis in children and adolescents is rare, usually is due to some comorbidities or medications, secondary osteoporosis. Surprisingly, no significant causes have been found for rare cases, idiopathic osteoporosis.
No matter what causes it, juvenile osteoporosis can be a significant problem because it occurs during the child’s prime bone-building years. From birth through young adulthood, children steadily accumulate bone mass, which peaks sometime before age 30. The greater their peak bone mass, the lower their risk for osteoporosis later in life. After people reach their mid thirties, bone mass typically begins to decline—very slowly at first but increasing in their fifties and sixties. Both heredity and lifestyle choices—especially the amount of calcium in the diet and the level of physical activity influence the development of peak bone mass and the rate at which bone is lost later in life.
Secondary Osteoporosis
- As the primary condition, juvenile idiopathic arthritis (also known as juvenile rheumatoid arthritis) provides a good illustration of the possible causes of secondary osteoporosis. In some cases, the disease process itself can cause osteoporosis.
- In other cases, medication used to treat the primary disorder may reduce bone mass. For example, drugs such as prednisone, used to treat severe cases of juvenile idiopathic arthritis, negatively affect bone mass.
- Finally, some behaviors associated with the primary disorder may lead to bone loss or reduction in bone formation. For example, a child with juvenile idiopathic arthritis may avoid physical activity, which is necessary for building and maintaining bone mass, because it may aggravate his or her condition or cause pain.[1]
Idiopathic Juvenile Osteoporosis
- Idiopathic juvenile osteoporosis (IJO) is a primary condition with no known cause. It is diagnosed after other causes of juvenile osteoporosis have been excluded. This rare form of osteoporosis typically occurs just before the onset of puberty in previously healthy children. The average age at onset is 7 years, with a range of 1 to 13 years. Most children experience complete recovery of bone.
- The first sign of IJO is usually pain in the lower back, hips, and feet, often accompanied by difficulty walking. Knee and ankle pain and fractures of the lower extremities also may occur. Physical malformations include kyphosis, loss of height, a sunken chest, or a limp. These physical malformations are sometimes reversible after IJO has run its course.
- X-rays of children with IJO often show low bone density, fractures of weight-bearing bones, and collapsed or misshapen vertebrae. However, conventional X-rays may not be able to detect osteoporosis until significant bone mass already has been lost. Newer methods such as dual energy x-ray absorptiometry (DXA), and quantitative computed tomography (QCT ) allow for earlier and more accurate diagnosis of low bone mass.
- There is no established medical or surgical therapy for juvenile osteoporosis. In some cases, no treatment may be needed because the condition usually goes away spontaneously. However, early diagnosis of juvenile osteoporosis is important so that steps can be taken to protect the child’s spine and other bones from fracture until remission occurs. These steps may include physical therapy, using crutches, avoiding unsafe weight-bearing activities, and other supportive care. A well-balanced diet rich in calcium and vitamin D is also important. In severe, long-lasting cases of juvenile osteoporosis, some medications called bisphosphonates, approved by the Food and Drug Administration for the treatment of osteoporosis in adults, have been given to children experimentally.
- Most children with IJO experience a complete recovery of bone tissue. Although growth may be somewhat impaired during the acute phase of the disorder, normal growth resumes—and catch-up growth often occurs—afterward. Unfortunately, in some cases, IJO can result in permanent disability such as kyphoscoliosis or collapse of the rib cage.[1]
Causes
Life Threatening Causes
Life-threatening causes include conditions which may result in death or permanent disability within 24 hours if left untreated. There are no life-threatening causes of osteoporosis, however complications resulting from untreated osteoporosis are common.
Common and Less Common Causes
FIRE: Focused Initial Rapid Evaluation
| Lifestyle modifications | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
| Exercise | Calcium Supplementation | Vitamin D supplementation | Smoking cessation | Reduced alcohol consumption | Hip protectors | Fall protection | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
| • Balance, strength and functional training exercises | Women • 9-18 yrs: 1,300 mg • 19-50 yrs: 1,000 mg • 51-70 yrs: 1,200 mg • 71 and more yrs: 1,200 mg Men • 50-70 yrs: 1,000 mg • 71 and more yrs: 1,200 mg | Women • 9-18 yrs: 600 IU • 19-50 yrs: 600 IU • 51-70 yrs: 600 IU • 71 and more yrs: 800 IU Men • More than 50 yrs: 800-1,000 IU • Serum vitamin D level of 20 ng per mL (50 nmol per L) is recommended for good bone health | • Stop-smoking program and nicotine patch | Limit to: • One drink/day for women • Two drinks/day for men • Moderate alcohol may associated with slightly higher BMD and lower fracture risk in postmenopausal women | • Hard and soft hip protectors, upon preference | Multifactorial interventions: • Individual risk assessment • Tai Chi and other exercise programs • Home safety assessment and modification by an occupational therapist • Gradual withdrawal of psychotropic medication • Visual impairment correction • Improve mobility | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
| Chronic glucocorticoid (GC) use | Children and adolescent | Adults | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
| Children | < 40 yrs | ≥ 40 yrs | Men | Women | |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
| Clinical fracture risk assessment*: • Within 6 months of the start of GC treatment • Every 12 months during GC treatment • No need to BMD measurement | As soon as possible but at least within 6 months of the initiation of GC treatment if: • High fracture risk • Significant osteoporotic risk factors (malnutrition, significant weight loss or low body weight, hypogonadism, secondary hyperparathyroidism, thyroid disease, family history of hip fracture, smoking, alcohol use) Every 2-3 yrs of GC treatment if: • Moderate-to-high fracture risk •• History of previous fracture •• BMD Z score <-3 •• Received very high-dose prednisone [≥30 mg/day and cumulative dose >5 gm] •• Risks for poor medication adherence or absorption •• Multiple osteoporotic risk factors | ≥ 40 yrs | • 18 yrs of age or 2 yrs after chemotherapy • Severe diseases • Low body weight • Chronic corticosteroid use • Delayed puberty • Gonadal failure • History of low-impact fracture | • Young hypogonadal • More than 70 yrs • Less than 70 yrs with: ••Low body weight ••Prior fracture ••High risk medication use ••Disease or condition associated with bone loss | • More than 65 yrs • Postmenopausal women younger than 65 yrs with: ••History of fragility fracture •• Weigh less than 127 lb (58 kg) ••Medications or diseases that cause bone loss •• Parental history of hip fracture •• smoking •• Alcoholism •• Rheumatoid arthritis. | ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Diagnosis
Treatment
Do's
Dont's
References
- ↑ 1.0 1.1 "Juvenile Osteoporosis".
- ↑ Krysiak R, Okopień B (2012). "[Pathogenesis and clinical presentation of andropause]". Pol. Merkur. Lekarski (in Polish). 32 (187): 70–3. PMID 22400185.
- ↑ Padova G, Borzì G, Incorvaia L, Siciliano G, Migliorino V, Vetri M, Tita P (2011). "Prevalence of osteoporosis and vertebral fractures in acromegalic patients". Clin Cases Miner Bone Metab. 8 (3): 37–43. PMC 3279059. PMID 22461828.
- ↑ Goswami M, Verma M, Singh A, Grewal H, Kumar G (2009). "Albright hereditary osteodystrophy: a rare case report". J Indian Soc Pedod Prev Dent. 27 (3): 184–8. doi:10.4103/0970-4388.57101. PMID 19841552.
- ↑ Pignolo RJ, Suda RK, McMillan EA, Shen J, Lee SH, Choi Y, Wright AC, Johnson FB (2008). "Defects in telomere maintenance molecules impair osteoblast differentiation and promote osteoporosis". Aging Cell. 7 (1): 23–31. doi:10.1111/j.1474-9726.2007.00350.x. PMC 2394673. PMID 18028256.
- ↑ Riminucci M, Collins MT, Corsi A, Boyde A, Murphey MD, Wientroub S, Kuznetsov SA, Cherman N, Robey PG, Bianco P (2001). "Gnathodiaphyseal dysplasia: a syndrome of fibro-osseous lesions of jawbones, bone fragility, and long bone bowing". J. Bone Miner. Res. 16 (9): 1710–8. doi:10.1359/jbmr.2001.16.9.1710. PMID 11547842.
- ↑ Nozaki T, Ihara K, Makimura M, Kinjo T, Hara T (2012). "A girl with Hajdu-Cheney syndrome and premature ovarian failure". J. Pediatr. Endocrinol. Metab. 25 (1–2): 171–3. PMID 22570971.
- ↑ Kaler SG, Garrity AM, Stern HJ, Rosenbaum KN, Orrison BM, Marini JC, Bernardini I, Saal HM (1992). "New autosomal recessive syndrome of sparse hair, osteopenia, and mental retardation in Mennonite sisters". Am. J. Med. Genet. 43 (6): 983–8. doi:10.1002/ajmg.1320430615. PMID 1415349.
- ↑ Kurtoglu S, Dundar M, Hallaç IK, Uzüm K, Okumuş Y, Oktem T (1997). "Polycystic kidney disease, biliary dysgenesis in a patient with Larsen's syndrome". Clin. Genet. 51 (6): 408–11. PMID 9237505.
- ↑ Tanaka H (2005). "[Systemic bone diseases; clues for the pathogenetic mechanism of osteoporosis]". Clin Calcium. 15 (5): 776–82. PMID 15876739.
- ↑ Gok F, Crettol LM, Alanay Y, Hacihamdioglu B, Kocaoglu M, Bonafe L, Ozen S (2010). "Clinical and radiographic findings in two brothers affected with a novel mutation in matrix metalloproteinase 2 gene". Eur. J. Pediatr. 169 (3): 363–7. doi:10.1007/s00431-009-1028-7. PMID 19653001.
- ↑ Khaldi F, Bennaceur B, Gharbi HA (1989). "[Familial osteochondrodysplatic dwarfism associated with deafness and tapeto-retinal heredo-degeneration]". Arch. Fr. Pediatr. (in French). 46 (6): 429–32. PMID 2783003.
- ↑ Heide T (1981). "[A syndrome of osteogenesis imperfecta, macrocephaly, wormian bones, frontal bossing, brachytelephalangy, hyperextensible joints, congenital blindness and oligophrenia in 3 sibs (author's transl)]". Klin Padiatr (in German). 193 (4): 334–40. doi:10.1055/s-2008-1034490. PMID 7265806.
- ↑ Hernández A, Nazará Z, Reynoso MC, Sarralde A, Bobadilla L, Fragoso R (1996). "Generalized osteoporosis in a patient with oculocutaneous hypopigmentation syndrome (OOCHS), without cerebral defects. A new syndrome?". Clin. Genet. 49 (1): 46–8. PMID 8721572.
- ↑ Gong Y, Vikkula M, Boon L, Liu J, Beighton P, Ramesar R, Peltonen L, Somer H, Hirose T, Dallapiccola B, De Paepe A, Swoboda W, Zabel B, Superti-Furga A, Steinmann B, Brunner HG, Jans A, Boles RG, Adkins W, van den Boogaard MJ, Olsen BR, Warman ML (1996). "Osteoporosis-pseudoglioma syndrome, a disorder affecting skeletal strength and vision, is assigned to chromosome region 11q12-13". Am. J. Hum. Genet. 59 (1): 146–51. PMC 1915094. PMID 8659519.
- ↑ Huq AH, Braverman RM, Greenberg F, Bacino CA, Rimoin DL, Lachman RS, Levin ML (1997). "The Pointer syndrome: a new syndrome with skeletal abnormalities, camptodactyly, facial anomalies, and feeding difficulties". Am. J. Med. Genet. 68 (2): 225–30. PMID 9028464.
- ↑ Gay BB, Kuhn JP (1976). "A syndrome of widened medullary cavities of bone, aortic calcification, abnormal dentition, and muscular weakness (the Singleton-Merten syndrome)". Radiology. 118 (2): 389–95. doi:10.1148/118.2.389. PMID 175395.
- ↑ Becerra-Solano LE, Butler J, Castañeda-Cisneros G, McCloskey DE, Wang X, Pegg AE, Schwartz CE, Sánchez-Corona J, García-Ortiz JE (2009). "A missense mutation, p.V132G, in the X-linked spermine synthase gene (SMS) causes Snyder-Robinson syndrome". Am. J. Med. Genet. A. 149A (3): 328–35. doi:10.1002/ajmg.a.32641. PMC 2653108. PMID 19206178.
- ↑ Lachman RS, Stoss H, Spranger J (1989). "Sponastrime dysplasia. A radiologic-pathologic correlation". Pediatr Radiol. 19 (6–7): 417–24. PMID 2771481.
- ↑ Rudolph G, Kalpadakis P, Bettecken T, Lichtner P, Haritoglou C, Hergersberg M, Meitinger T, Schmidt H (2003). "Spondylo-ocular syndrome: a new entity with crystalline lens malformation, cataract, retinal detachment, osteoporosis, and platyspondyly". Am. J. Ophthalmol. 135 (5): 681–7. PMID 12719077.
- ↑ Jeong SY, Kim BY, Kim HJ, Yang JA, Kim OH (2010). "A novel homozygous MMP2 mutation in a patient with Torg-Winchester syndrome". J. Hum. Genet. 55 (11): 764–6. doi:10.1038/jhg.2010.102. PMID 20720557.
- ↑ Delépine M, Nicolino M, Barrett T, Golamaully M, Lathrop GM, Julier C (2000). "EIF2AK3, encoding translation initiation factor 2-alpha kinase 3, is mutated in patients with Wolcott-Rallison syndrome". Nat. Genet. 25 (4): 406–9. doi:10.1038/78085. PMID 10932183.
- ↑ Boente Mdel C, Asial RA, Winik BC (2006). "Geroderma osteodysplastica. Report of a new family". Pediatr Dermatol. 23 (5): 467–72. doi:10.1111/j.1525-1470.2006.00285.x. PMID 17014644.
- ↑ Hennekam RC (2006). "Hutchinson-Gilford progeria syndrome: review of the phenotype". Am. J. Med. Genet. A. 140 (23): 2603–24. doi:10.1002/ajmg.a.31346. PMID 16838330.
- ↑ Nojiri H, Saita Y, Morikawa D, Kobayashi K, Tsuda C, Miyazaki T, Saito M, Marumo K, Yonezawa I, Kaneko K, Shirasawa T, Shimizu T (2011). "Cytoplasmic superoxide causes bone fragility owing to low-turnover osteoporosis and impaired collagen cross-linking". J. Bone Miner. Res. 26 (11): 2682–94. doi:10.1002/jbmr.489. PMID 22025246.
- ↑ Lekva T, Ueland T, Bøyum H, Evang JA, Godang K, Bollerslev J (2012). "TXNIP is highly regulated in bone biopsies from patients with endogenous Cushing's syndrome and related to bone turnover". Eur. J. Endocrinol. 166 (6): 1039–48. doi:10.1530/EJE-11-1082. PMID 22450549.
- ↑ Ferlin A, Schipilliti M, Foresta C (2011). "Bone density and risk of osteoporosis in Klinefelter syndrome". Acta Paediatr. 100 (6): 878–84. doi:10.1111/j.1651-2227.2010.02138.x. PMID 21214887.
- ↑ Grasswick LJ, Bradford JM (2003). "Osteoporosis associated with the treatment of paraphilias: a clinical review of seven case reports". J. Forensic Sci. 48 (4): 849–55. PMID 12877306.
- ↑ Vasireddy S, Swinson DR (2001). "Male osteoporosis associated with longterm cyproterone treatment". J. Rheumatol. 28 (7): 1702–3. PMID 11469484.
- ↑ Saltzstein RJ, Hardin S, Hastings J (1992). "Osteoporosis in spinal cord injury: using an index of mobility and its relationship to bone density". J Am Paraplegia Soc. 15 (4): 232–4. PMID 1431871.
- ↑ Gold DT, Solimeo S (2006). "Osteoporosis and depression: a historical perspective". Curr Osteoporos Rep. 4 (4): 134–9. PMID 17112423.
- ↑ Delsignore JL, Dvoretsky PM, Hicks DG, O'Keefe RJ, Rosier RN (1996). "Mastocytosis presenting as a skeletal disorder". Iowa Orthop J. 16: 126–34. PMC 2378151. PMID 9129284.
- ↑ Dytfeld J, Horst-Sikorska W (2012). "Pregnancy associated osteoporosis--a case report". Ginekol. Pol. 83 (5): 377–9. PMID 22708337.
- ↑ Elshal MF, Bernawi AE, Al-Ghamdy MA, Jalal JA (2012). "The association of bone mineral density and parathyroid hormone with serum magnesium in adult patients with sickle-cell anaemia". Arch Med Sci. 8 (2): 270–6. doi:10.5114/aoms.2012.28554. PMC 3361039. PMID 22662000.