Marfan syndrome: Difference between revisions

"Marfan" redirects here. For the man who discovered the syndrome, see Antoine Marfan.

Marfan syndrome
Specialty	Medical genetics

Marfan syndrome (also called Marfan's syndrome) is a genetic disorder of the connective tissue.

It is sometimes inherited as a dominant trait. It is carried by a gene called FBN1, which encodes a connective protein called fibrillin-1.^[1][2] People have a pair of FBN1 genes. Because it is dominant, people who have inherited one affected FBN1 gene from either parent will have Marfan's. This syndrome can run from mild to severe.

People with Marfan's are typically tall, with long limbs and long thin fingers.

The most serious complications are the defects of the heart valves and aorta. It may also affect the lungs, eyes, the dural sac surrounding the spinal cord, skeleton and the hard palate.

In addition to being a connective protein that forms the structural support for tissues outside the cell, the normal fibrillin-1 protein binds to another protein, transforming growth factor beta (TGF-β).^[2] TGF-β has deleterious effects on vascular smooth muscle development and the integrity of the extracellular matrix. Researchers now believe that secondary to mutated fibrillin there is excessive TGF-β at the lungs, heart valves, and aorta, and this weakens the tissues and causes the features of Marfan syndrome.^[3] Since angiotensin II receptor blockers (ARBs) also reduce TGF-β, they have tested this by giving ARBs (losartan, etc.) to a small sample of young, severely affected Marfan syndrome patients. In some patients, the growth of the aorta was indeed reduced.^[4]

It is named after Antoine Marfan,^[5] the French pediatrician who first described the condition in 1896 after noticing striking features in a 5-year-old girl.^[6][7] The gene linked to the disease was first identified by Francesco Ramirez at the Mount Sinai Medical Center in New York City in 1991.^[8]

Symptoms

Although there are no unique signs or symptoms of Marfan syndrome, the constellation of long limbs, dislocated lenses, and aortic root dilation is sufficient to make the diagnosis with confidence. There are more than 30 other clinical features that are variably associated with the syndrome, most involving the skeleton, skin, and joints. There is a great deal of clinical variability even within families that carry the identical mutation.

Skeletal system

The most of readily visible signs are associated with the skeletal system. Many individuals with Marfan syndrome grow to above average height. Some have long slender limbs with long fingers and toes (arachnodactyly). This condition of elongated limbs is known as dolichostenomelia. An individual's arms may be disproportionately long, with thin, weak wrists. In addition to affecting height and limb proportions, Marfan syndrome can produce other skeletal anomalies. Abnormal curvature of the spine (scoliosis) is common, as is abnormal indentation (pectus excavatum) or protrusion (pectus carinatum) of the sternum. Other signs include abnormal joint flexibility, a high palate, malocclusions, flat feet, hammer toes, stooped shoulders, unexplained stretch marks on the skin. It can also cause pain in the joints, bones and muscles in some patients. Some people with Marfan have speech disorders resulting from symptomatic high palates and small jaws. Early osteoarthritis may occur.

Eyes

Lens dislocation in Marfan's syndrome, the lens was kidney-shaped and was resting against the ciliary body.

Marfan syndrome can also seriously affect the eyes and vision. Nearsightedness and astigmatism are common, but farsightedness can also result. Subluxation (dislocation) of the crystalline lens in one or both eyes (ectopia lentis) (in 80% of patients) also occurs and may be detected by an ophthalmologist or optometrist using a slit-lamp biomicroscope. In Marfan's the dislocation is typically superotemporal whereas in the similar condition homocystinuria, the dislocation is inferonasal. Sometimes eye problems appear only after the weakening of connective tissue has caused detachment of the retina.^[9] Early onset glaucoma can be another related problem.

Cardiovascular system

The most serious signs and symptoms associated with Marfan syndrome involve the cardiovascular system. Undue fatigue, shortness of breath, heart palpitations, racing heartbeats, or Angina pectoris with pain radiating to the back, shoulder, or arm. Cold arms, hands and feet can also be linked to Marfan's syndrome because of inadequate circulation. A heart murmur, abnormal reading on an EKG, or symptoms of angina can indicate further investigation. The signs of regurgitation from prolapse of the mitral or aortic valves (which control the flow of blood through the heart) result from cystic medial degeneration of the valves which is commonly associated with Marfan's syndrome (see mitral valve prolapse, aortic regurgitation). However, the major sign that would lead a doctor to consider an underlying condition is a dilated aorta or an aortic aneurysm. Sometimes, no heart problems are apparent until the weakening of the connective tissue (cystic medial degeneration) in the ascending aorta causes an aortic aneurysm or aortic dissection, a surgical emergency. An aortic dissection is most often fatal and presents with pain radiating down the back, giving a tearing sensation.

Because of the underlying connective tissue abnormalities that cause Marfan syndrome, there is an increased incidence of dehiscence of prosthetic mitral valve.^[10] Care should be taken to attempt repair of damaged heart valves rather than replacement.

During pregnancy, even in the absence of preconceived cardiovascular abnormality, women with Marfan syndrome are at significant risk of aortic dissection, which is often fatal even when rapidly treated. For this reason, women with Marfan syndrome should receive a thorough assessment prior to conception, and echocardiography should be performed every six to ten weeks during pregnancy, to assess the aortic root diameter. For most women, safe vaginal delivery is possible.^[11]

Lungs

Marfan syndrome is a risk factor for spontaneous pneumothorax. In spontaneous unilateral pneumothorax, air escapes from a lung and occupies the pleural space between the chest wall and a lung. The lung becomes partially compressed or collapsed. This can cause pain, shortness of breath, cyanosis, and, if not treated, death. Marfan syndrome has also been associated with sleep apnea and idiopathic obstructive lung disease.

Central nervous system

Another condition that can reduce the quality of life for an individual, though not life-threatening, is dural ectasia, the weakening of the connective tissue of the dural sac, the membrane that encases the spinal cord. Dural ectasia can be present for a long time without producing any noticeable symptoms. Symptoms that can occur are lower back pain, leg pain, abdominal pain, other neurological symptoms in the lower extremities, or headaches. Such symptoms usually diminish when the individual lies flat on his or her back. These types of symptoms might lead a doctor to order an X-ray of the lower spine. Dural ectasia is usually not visible on an X-ray in the early phases. A worsening of symptoms and the lack of finding any other cause should eventually lead a doctor to order an upright MRI of the lower spine. Dural ectasia that has progressed to the point of causing these symptoms would appear in an upright MRI image as a dilated pouch that is wearing away at the lumbar vertebrae.^[9] Other spinal issues associated with Marfan include degenerative disk disease and spinal cysts. Marfan syndrome is also associated with dysautonomia.

Pathogenesis

Marfan syndrome is caused by mutations in the FBN1 gene on chromosome 15,^[12] which encodes a glycoprotein called fibrillin-1, a component of the extracellular matrix. The Fibrillin 1 protein is essential for the proper formation of the extracellular matrix including the biogenesis and maintenance of elastic fibers. The extracellular matrix is critical for both the structural integrity of connective tissue but also serves as a reservoir for growth factors.^[13] Elastin fibers are found throughout the body but are particularly abundant in the aorta, ligaments and the ciliary zonules of the eye; consequently, these areas are among the worst affected.

A transgenic mouse has been created carrying a single copy of a mutant fibrillin 1, a mutation similar to that found in the human fibrillin 1 gene that is known to cause Marfan syndrome. This mouse strain recapitulates many of the features of the human disease and promises to provide insights into the pathogenesis of the disease. Reducing the level of normal fibrillin-1 causes a Marfan-related disease in mice.^[14]

Transforming growth factor beta (TGFβ) plays an important role in Marfan syndrome. Fibrillin-1 indirectly binds a latent form of TGFβ keeping it sequestered and unable to exert its biological activity. The simplest model of Marfan syndrome suggests that reduced levels of fibrillin-1 allow TGFβ levels to rise due to inadequate sequestration. Although it is not proven how elevated TGFβ levels are responsible for the specific pathology seen with the disease, an inflammatory reaction releasing proteases that slowly degrade the elastin fibers and other components of the extracellular matrix is known to occur. The importance of the TGFβ pathway was confirmed with the discovery of a similar syndrome Loeys-Dietz syndrome involving the TGFβR2 gene on chromosome 3, a receptor protein of TGFβ.^[15] Marfan syndrome has often been confused with Loeys-Dietz syndrome, because of the considerable clinical overlap between the two syndromes.^[16]

Diagnosis

Diagnostic criteria of Marfan syndrome were agreed internationally in 1996.^[17] A diagnosis of Marfan syndrome is based on family history and a combination of major and minor indicators of the disorder, rare in the general population, that occur in one individual. For example: four skeletal signs with one or more signs in another body system such as ocular and cardiovascular in one individual. The following conditions may result from Marfan syndrome but may also occur in people without any known underlying disorder.

• Aortic aneurysm or dilation
• Arachnodactyly
• GERD
• Bicuspid aortic valve
• Cysts
• Cystic medial necrosis
• Deviated septum^[18]
• Dural ectasia
• Early cataracts
• Early glaucoma^[19]
• Early osteoarthritis^[20]
• Ectopia lentis
• Emphysema^[21]

• Eye iris coloboma^[22]
• Flat feet
• Above-average height
• Heart palpitations^[23]
• Hernias
• Hypermobility of the joints
• Kyphosis (hunched back)
• Leaky heart valve
• Malocclusion
• Micrognathia (small lower jaw)^[22]
• Mitral valve prolapse
• Myopia (near sightedness)

• Obstructive lung disease
• Osteopenia (low bone density)^[24]
• Pectus carinatum or excavatum
• Pneumothorax (collapsed lung)
• Retinal detachment
• Scoliosis
• Sleep apnea
• Stretch marks not from pregnancy^[25] or obesity
• Teeth crowded^[25]
• "Narrow, thin face"^[22]
• Temporomandibular joint disorder (TMD)^[26]

Differential diagnosis

The following disorders have similar signs and symptoms of Marfan syndrome:

• Congenital Contractural Arachnodactyly (CCA) or Beals Syndrome
• Ehlers-Danlos syndrome
• Homocystinuria
• Loeys-Dietz syndrome
• MASS phenotype
• Shprintzen-Goldberg syndrome ^[27]
• Stickler syndrome
• Multiple endocrine neoplasia, type 2B

Management

There is no cure for Marfan syndrome, but life expectancy has increased significantly over the last few decades, and clinical trials are underway for a promising new treatment.^[28] The syndrome is treated by addressing each issue as it arises, and, in particular, considering preventive medication, even for young children, to slow progression of aortic dilation.

Regular checkups by a cardiologist are needed to monitor the health of the heart valves and the aorta. The goal of treatment is to slow the progression of aortic dilation and damage to heart valves by eliminating arrythmias, minimizing the heart rate, and minimizing blood pressure. Beta blockers have been used to control arrythmias and slow the heart rate. Other medications might be needed to further minimize blood pressure without slowing the heart rate, such as ACE inhibitors and angiotensin II receptor antagonists, also known as angiontensin receptor blockers (ARBs). If the dilation of the aorta progresses to a significant diameter aneurysm, causes a dissection or a rupture, or leads to failure of the aortic or other valve, then surgery (possibly a composite aortic valve graft [CAVG] or valve-sparing procedure) becomes necessary. Although aortic graft surgery (or any vascular surgery) is a serious undertaking it is generally successful if undertaken on an elective basis.^[29] Surgery in the setting of acute aortic dissection or rupture is considerably more problematic. Elective aortic valve/graft surgery is usually considered when aortic root diameter reaches 50 millimeters (2.0 inches), but each case needs to be specifically evaluated by a qualified cardiologist. New valve-sparing surgical techniques are becoming more common.^[30] As Marfan patients live longer, other vascular repairs are becoming more common, e.g., repairs of descending thoractic aortic aneurysms and aneurysms of vessels other than the aorta.

The skeletal and ocular manifestations of Marfan syndrome can also be serious, although not life-threatening. These symptoms are usually treated in the typical manner for the appropriate condition, such as with various kinds of pain medication or muscle relaxants. It is also common for patients to receive treatment from a physiotherapist, using TENS therapy, ultrasound and skeletal adjustment.^{[citation needed]} This can also affect height, arm length, and life span. A physiotherapist can also help improve function and prevent injuries in individuals with Marfan's. The Nuss procedure is now being offered to people with Marfan syndrome to correct 'sunken chest' or (pectus excavatum).^[31] Because Marfan may cause spinal abnormalities that are asymptomatic, any spinal surgery contemplated on a Marfan patient should only follow detailed imaging and careful surgical planning, regardless of the indication for surgery.

Treatment of a spontaneous pneumothorax is dependent on the volume of air in the pleural space and the natural progression of the individual's condition. A small pneumothorax might resolve without active treatment in one to two weeks. Recurrent pneumothoraces might require chest surgery. Moderately sized pneumothoraces might need chest drain management for several days in a hospital. Large pneumothoraces are likely to be medical emergencies requiring emergency decompression.

Research in laboratory mice has suggested that the angiotensin II receptor antagonist losartan, which appears to block TGF-beta activity, can slow or halt the formation of aortic aneurysms in Marfan syndrome.^[32] A large clinical trial sponsored by the National Institutes of Health comparing the effects of losartan and atenolol on the aortas of Marfan patients was scheduled to begin in early 2007, coordinated by Johns Hopkins.^[33]

Genetic counseling and specialized clinics are available at many academic medical centers for affected persons and family members.

Epidemiology

Marfan syndrome affects males and females equally,^[34] and the mutation shows no ethnic or geographical bias.^[35] Estimates indicate that approximately 1 in 3,000 to 5,000 individuals have Marfan syndrome.^[35] Each parent with the condition has a 50% risk of passing the genetic defect on to any child due to its autosomal dominant nature. Most individuals with Marfan syndrome have another affected family member, but approximately 15–30% of all cases are due to de novo genetic mutations^[13]—such spontaneous mutations occur in about 1 in 20,000 births. Marfan syndrome is also an example of dominant negative mutation and haploinsufficiency.^[36][37] It is associated with variable expressivity; incomplete penetrance has not been definitively documented.

Well-known people

Prominent figures who have been diagnosed with Marfan syndrome include:

• Bradford Cox,^[38] frontman of the bands Deerhunter and Atlas Sound
• Flo Hyman,^[39] silver medal in Women's Volleyball (1984 Olympics)
• Jonathan Larson,^[40] author and composer of the hit musical Rent
• Joey Ramone,^[41] singer for punk rock band The Ramones
• Vincent Schiavelli,^[42] actor
• Sir John Tavener,^[43] contemporary British composer

Speculative claims concerning historical figures

The diagnosis of Marfan syndrome was not available until well into the 20th century, but there has been speculation on whether historical figures may have had it, based on sparse medical records, descriptions, and images. Ancient figures include Akhenaten, Egyptian pharaoh, based on his image in early Amarna art.^[44] Musicians and composers Niccolò Paganini^[45], Sergei Rachmaninoff^[46], and Robert Johnson ^[47] are thought by some to have had the disease. A 1962 theory that Abraham Lincoln had Marfan syndrome has little currency today.^[48][49] According to a 2007 theory, it is more likely that he had a different disorder, multiple endocrine neoplasia type 2B, that caused skeletal features almost identical to Marfan syndrome.^[50]

References

1. Kainulainen K, Karttunen L., Puhakka L, Sakai L, Peltonen L. Mutations in the fibrillin gene responsible for dominant ectopia lentis and neonatal Marfan syndrome. Nat Genet 1994; 6: 64-9.
2. Dietz HC, Loeys B, Carta L, Ramirez F. Recent progress towards a molecular understanding of Marfan syndrome. Am J Med Genet C Semin Med Genet 2005; 139: 4-9.
3. Robbins and Cotran Pathological Basis of Disease, Kumar et al; 8th Edition, Saunders Elsevier Publishing, 2010
4. Pyeritz RE (2008). "A small molecule for a large disease". N. Engl. J. Med. 358 (26): 2829–31. doi:10.1056/NEJMe0804008. PMID 18579819. {{cite journal}}: Unknown parameter |month= ignored (help)
5. Template:Fr icon Marfan, Antoine (1896). "Un cas de déformation congénitale des quartre membres, plus prononcée aux extrémitiés, caractérisée par l'allongement des os avec un certain degré d'amincissement [A case of congenital deformation of the four limbs, more pronounced at the extremities, characterized by elongation of the bones with some degree of thinning]". Bulletins et memoires de la Société medicale des hôspitaux de Paris. 13 (3rd series): 220–226.
6. Johns Hopkins Comprehensive Marfan Center. John Hopkins Medicine. Retrieved on January 6, 2009.
7. Antoine Bernard-Jean Marfan. Who Named It? Retrieved on January 20, 2009.
8. Brown P (July 27, 1991). "Marfan syndrome linked to gene". New Scientist. Retrieved on August 11, 2008.
9. "Marfan Syndrome". Mayo Clinic. Retrieved January 12, 2007. {{cite web}}: Unknown parameter |dateformat= ignored (help)
10. Braunwald's Heart Disease ~ A Textbook of Cardiovascular Medicine, Seventh Edition. United States of America: Elseview Saunders. 2005. p. 1894. ISBN 0-7216-0509-5. {{cite book}}: Unknown parameter |coauthors= ignored (|author= suggested) (help)
11. Chen H (June 4, 2007). "Marfan Syndrome". eMedicine. Retrieved June 25, 2007. {{cite web}}: Unknown parameter |dateformat= ignored (help)
12. McKusick V (1991). "The defect in Marfan syndrome". Nature. 352 (6333): 279–81. doi:10.1038/352279a0. PMID 1852198.
13. Cotran (1998). Robbins Pathologic Basis of Disease. Philadelphia: W.B Saunders Company. ISBN 0-7216-7335-X. {{cite book}}: Unknown parameter |coauthors= ignored (|author= suggested) (help)
14. Pereira L, Lee SY, Gayraud B; et al. (1999). "Pathogenetic sequence for aneurysm revealed in mice underexpressing fibrillin-1". Proceedings of the National Academy of Sciences of the United States of America. 96 (7): 3819–23. doi:10.1073/pnas.96.7.3819. PMC 22378. PMID 10097121. {{cite journal}}: Explicit use of et al. in: |author= (help); Unknown parameter |month= ignored (help)
15. Entrez Gene (2007). "TGFBR2 transforming growth factor, beta receptor II" (Entrez gene entry). NCBI. Retrieved January 11, 2007. {{cite web}}: Unknown parameter |dateformat= ignored (help)
16. "Related Disorders: Loeys-Dietz". National Marfan Foundation. Retrieved January 11, 2007. {{cite web}}: Unknown parameter |dateformat= ignored (help)
17. De Paepe A, Devereux RB, Dietz HC, Hennekam RCM, Pyeritz RE. Revised diagnostic criteria for the Marfan syndrome. Am J Med Genet 1996; 62: 417-26.
18. Finkbohner R, Johnston D, Crawford ES, Coselli J, Milewicz DM (1995). "Marfan syndrome. Long-term survival and complications after aortic aneurysm repair". Circulation. 91 (3): 728–33. PMID 7828300. {{cite journal}}: Unknown parameter |month= ignored (help)
19. "Marfan Syndrome - Signs and Symptoms". www.ucsfhealth.org. Retrieved 2009-08-28.
20. "The Marfan Trust - What is Marfan Syndrome?". www.marfantrust.org. Retrieved 2009-08-28.
21. "Marfan Syndrome: The Similarities to Copper Deficiency". www.ctds.info. Retrieved 2009-08-29.
22. "Marfan syndrome: MedlinePlus Medical Encyclopedia". www.nlm.nih.gov. Retrieved 2009-08-28.
23. "Marfan syndrome - Genetics Home Reference". ghr.nlm.nih.gov. Retrieved 2009-08-28.
24. Kohlmeier L, Gasner C, Bachrach LK, Marcus R (1995). "The bone mineral status of patients with Marfan syndrome". Journal of Bone and Mineral Research. 10 (10): 1550–5. PMID 8686512. {{cite journal}}: Unknown parameter |month= ignored (help)
25. "About Marfan Syndrome: Features". National Marfan Foundation. Retrieved 2009-08-28.
26. "Living with Marfan Syndrome: Dental issues". National Marfan Foundation. Retrieved 2009-08-28.
27. "Shprintzen-Goldberg Syndrome -- GeneReviews -- NCBI Bookshelf". www.ncbi.nlm.nih.gov. Retrieved 2009-08-29.
28. Freeman, Elaine (2007) "A Silver Bullet for Blake", Johns Hopkins Magazine, Fall, 2007.
29. "Elective Aortic Root Surgery in Marfan Syndrome Appears Safe and Durable: Presented at STS" (Press release). Doctor's Guide. January 31, 2008. Retrieved January 13, 2009.
    See also:
    • Cameron DE, Vricella LA (2005). "Valve-sparing aortic root replacement in Marfan syndrome". Seminars in Thoracic and Cardiovascular Surgery. 8: 103–11. doi:10.1053/j.pcsu.2005.03.001. PMID 15818365.
    • Gott VL, Cameron DE, Alejo DE; et al. (2002). "Aortic root replacement in 271 Marfan patients: a 24-year experience". The Annals of Thoracic Surgery. 73 (2): 438–43. doi:10.1016/S0003-4975(01)03336-7. PMID 11845856. {{cite journal}}: Explicit use of et al. in: |author= (help); Unknown parameter |month= ignored (help)
    • Bethea BT, Fitton TP, Alejo DE; et al. (2004). "Results of aortic valve-sparing operations: experience with remodeling and reimplantation procedures in 65 patients". The Annals of Thoracic Surgery. 78 (3): 767–72, discussion 767–72. doi:10.1016/j.athoracsur.2004.03.040. PMID 15336989. {{cite journal}}: Explicit use of et al. in: |author= (help); Unknown parameter |month= ignored (help)
30. "Heart Surgery for Marfan Syndrome". Mayo Clinic. Retrieved January 12, 2007. {{cite web}}: Unknown parameter |dateformat= ignored (help)
31. "Overview of the Nuss Procedure for Pectus Excavatum". Children's Hospital of The King's Daughters. Retrieved January 12, 2007. {{cite web}}: Unknown parameter |dateformat= ignored (help)
32. Habashi JP, Judge DP, Holm TM; et al. (2006). "Losartan, an AT1 antagonist, prevents aortic aneurysm in a mouse model of Marfan syndrome". Science. 312 (5770): 117–21. doi:10.1126/science.1124287. PMC 1482474. PMID 16601194. {{cite journal}}: Explicit use of et al. in: |author= (help); Unknown parameter |month= ignored (help)
33. "Atenolol vs. Losartan in Individuals with Marfan Syndrome Clinial Trial". National Marfan Foundation. Retrieved January 12, 2007. {{cite web}}: Unknown parameter |dateformat= ignored (help)
34. Fusar-Poli P, Klersy C, Stramesi F, Callegari A, Arbustini E, Politi P (2008). "Determinants of quality of life in Marfan syndrome". Psychosomatics. 49 (3): 243–8. doi:10.1176/appi.psy.49.3.243. PMID 18448780.
35. Keane MG, Pyeritz RE (2008). "Medical management of Marfan syndrome". Circulation. 117 (21): 2802–13. doi:10.1161/CIRCULATIONAHA.107.693523. PMID 18506019. {{cite journal}}: Unknown parameter |month= ignored (help)
36. Judge DP, Biery NJ, Keene DR; et al. (2004). "Evidence for a critical contribution of haploinsufficiency in the complex pathogenesis of Marfan syndrome". The Journal of Clinical Investigation. 114 (2): 172–81. doi:10.1172/JCI20641. PMC 449744. PMID 15254584. {{cite journal}}: Explicit use of et al. in: |author= (help); Unknown parameter |month= ignored (help)
37. Judge DP, Dietz HC (2005). "Marfan's syndrome". Lancet. 366 (9501): 1965–76. doi:10.1016/S0140-6736(05)67789-6. PMC 1513064. PMID 16325700. {{cite journal}}: Unknown parameter |month= ignored (help)
38. Schreiber R (June 11, 2007). "Pitchfork Feature: Interview: Deerhunter". Retrieved January 6, 2009. {{cite web}}: Unknown parameter |dateformat= ignored (help)
39. "Flo Hyman". Volleyball Hall of Fame. Archived from the original on January 30, 2008. Retrieved January 6, 2009. {{cite web}}: Unknown parameter |dateformat= ignored (help)
40. "Marfan Syndrome Community Benefits from the Legacy of Jonathan Larson, RENT Playwright". National Marfan Foundation. Retrieved January 6, 2009. {{cite web}}: Unknown parameter |dateformat= ignored (help)
41. "Joey Ramone". The Independent. March 18, 2008. Retrieved January 6, 2008.
42. "NMF Mourns the Loss of its Honorary Co-Chair, Vincent Schiavelli". National Marfan Foundation. Retrieved January 6, 2009. {{cite web}}: Unknown parameter |dateformat= ignored (help)
43. Morrison R (November 2004). 99 Names for God: John Tavener turns his back on Orthodoxy, BBC Music, page 30
44. "Did Akhenaten Suffer from Marfan's Syndrome?". Canadian Marfan Association. Retrieved January 6, 2009. {{cite web}}: Unknown parameter |dateformat= ignored (help)
45. From Paganini stories myths. The AFU and Urban Legends Archive. Retrieved on January 13, 2009; based primarily on Schoenfeld MR (1978). "Nicolo Paganini. Musical magician and Marfan mutant?". JAMA. 239 (1): 40–2. doi:10.1001/jama.239.1.40. PMID 336919. {{cite journal}}: Unknown parameter |month= ignored (help)
46. Wolf P (2001). "Creativity and chronic disease. Sergei Rachmaninov (1873-1943)". West. J. Med. 175 (5): 354. doi:10.1136/ewjm.175.5.354. PMC 1071626. PMID 11694497. {{cite journal}}: Unknown parameter |month= ignored (help)
47. Connel D (September 2, 2006). "Retrospective blues: Robert Johnson—an open letter to Eric Clapton". British Medical Journal. 333 (7566): 489. doi:10.1136/bmj.333.7566.489. Retrieved January 11, 2007.
48. Marfan syndrome. MayoClinic.com. Retrieved on January 6, 2009.
49. Aneurysm and dissection of the aorta. NIH. Retrieved on January 6, 2009.
50. From The Last - and Greatest - Lincoln Mystery. The Physical Lincoln. Retrieved on January 13, 2009; reporting on Sotos JG (2008). The Physical Lincoln. Mt. Vernon Book Systems. ISBN 9780981819327

External links

• Marfan syndrome at Curlie
• Marfan Syndrome Diagnosis (www.nature.com)
• Marfan syndrome - NIH's Office of Rare Diseases
• GeneReviews/NCBI/UW/NIH entry on Marfan syndrome
• GeneReviews/NCBI/NIH/UW entry on Shprintzen-Goldberg Syndrome