“Coronary stent”的意思、由来-开放百科全书

A coronary stent is a tube-shaped device placed in the coronary arteries that supply blood to the heart, to keep the arteries open in the treatment of coronary heart disease. It is used in a procedure called percutaneous coronary intervention (PCI). Coronary stents are now used in more than 90% of PCI procedures.^[1] Stents reduce angina (chest pain) and have been shown to improve survivability and decrease adverse events in an acute myocardial infarction.^[2]^[3]

Similar stents and procedures are used in non-coronary vessels (e.g., in the legs in peripheral artery disease).

Medical uses

Treating a blocked ("stenosed") coronary artery with a stent follows the same steps as other angioplasty procedures with a few important differences. The interventional cardiologist uses angiography to assess the location and estimate the size of the blockage ("lesion") by injecting a contrast medium through the guide catheter and viewing the flow of blood through the downstream coronary arteries. Intravascular ultrasound (IVUS) may be used to assess the lesion's thickness and hardness ("calcification"). The cardiologist uses this information to decide whether to treat the lesion with a stent and if so, what kind and size. Drug-eluting stents are most often sold as a unit, with the stent in its collapsed form attached to the outside of a balloon catheter. Outside the US, physicians may perform "direct stenting", where the stent is threaded through the lesion and expanded. Common practice in the US is to predilate the blockage before delivering the stent. Predilation is accomplished by threading the lesion with an ordinary balloon catheter and expanding it to the vessel's original diameter. The physician withdraws this catheter and threads the stent on its balloon catheter through the lesion. The physician expands the balloon, which deforms the metal stent to its expanded size. The cardiologist may "customize" the fit of the stent to match the blood vessel's shape, using IVUS to guide the work.^[4] It is critically important that the framework of the stent be in direct contact with the walls of the vessel to minimize potential complications such as blood clot formation. Very long lesions may require more than one stent—the result of this treatment is sometimes referred to as a "full metal jacket".^[5]

The procedure itself is performed in a catheterization clinic ("cath lab"). Barring complications, patients undergoing catheterizations are kept at least overnight for observation.^[6]

Dealing with lesions near branches in the coronary arteries presents additional challenges and requires additional techniques.^[7]

Risks

Though the chances of having complications from a PCI are small, some serious complications include the development of arrythmias, adverse reactions/effects of the dye used in the procedure, infection, restenosis, clotting, blood vessel damage, and bleeding at catheter insertion site.^[8]

Re-occlusion

Coronary artery stents, typically a metal framework, can be placed inside the artery to help keep it open. However, as the stent is a foreign object (not native to the body), it incites an immune response. This may cause scar tissue (cell proliferation) to rapidly grow over the stent. In addition, there is a strong tendency for clots to form at the site where the stent damages the arterial wall, if such damage happens. Since platelets are involved in the clotting process, patients must take dual antiplatelet therapy starting immediately before or after stenting: usually an ADP receptor antagonist (e.g. clopidogrel or ticagrelor) and aspirin for up to one year and aspirin indefinitely.^[9]^[1]

However, in some cases the dual antiplatelet therapy may be insufficient to fully prevent clots that may result in stent thrombosis; these clots and cell proliferation may sometimes cause standard (“bare-metal”) stents to become blocked (restenosis). Drug-eluting stents were developed with the intent of dealing with this problem: by releasing an antiproliferative drug (drugs typically used against cancer or as immunosuppressants), they can help reduce the incidence of "in-stent restenosis" (re-narrowing).

Restenosis

One of the drawbacks of vascular stents is the potential for restenosis via the development of a thick smooth muscle tissue inside the lumen, the so-called neointima. Development of a neointima is variable but can at times be so severe as to re-occlude the vessel lumen (restenosis), especially in the case of smaller-diameter vessels, which often results in reintervention. Consequently, current research focuses on the reduction of neointima after stent placement. Substantial improvements have been made, including the use of more biocompatible materials, anti-inflammatory drug-eluting stents, resorbable stents, and others. Restenosis can be treated with a reintervention using the same method.

Controversy

The value of stenting in rescuing someone having a heart attack (by immediately alleviating an obstruction) is clearly defined in multiple studies, but studies have failed to find reduction in hard endpoints for stents vs. medical therapy in stable angina patients (see below). The artery-opening stent can temporarily alleviate chest pain, but does not contribute to longevity. The "...vast majority of heart attacks do not originate with obstructions that narrow arteries." Further, “...researchers say, most heart attacks do not occur because an artery is narrowed by plaque. Instead, they say, heart attacks occur when an area of plaque bursts, a clot forms over the area and blood flow is abruptly blocked. In 75 to 80 percent of cases, the plaque that erupts was not obstructing an artery and would not be stented or bypassed. The dangerous plaque is soft and fragile, produces no symptoms and would not be seen as an obstruction to blood flow.”^[11]

A more permanent and successful way to prevent heart attacks in patients at high risk is to give up smoking, to exercise regularly, and take "drugs to get blood pressure under control, drive cholesterol levels down and prevent blood clotting".^[10]

Some cardiologists believe that stents are overused; however, in certain patient groups, such as the elderly, GRACE and other studies have found evidence of under-use. One cardiologist was convicted of billing patients for performing medically unnecessary stenting.^[11]^[12] Guidelines recommend a stress test before implanting stents, but most patients do not receive a stress test.^[13]

Research

While revascularisation (by stenting or bypass surgery) is of clear benefit in reducing mortality and morbidity in patients with acute symptoms (acute coronary syndromes) including myocardial infarction, their benefit is less marked in stable patients. Clinical trials have failed to demonstrate that coronary stents improve survival over best medical treatment.

Several other clinical trials have been performed to examine the efficacy of coronary stenting and compare with other treatment options. A consensus of the medical community does not exist.

History

The first stent was patented in 1972 by Robert A. Ersek, MD based on work he had done in animals in 1969 at the University of Minnesota. In addition to intervascular stents, he also developed the first stent-supported porcine valve that can be implanted transcutaneously in 7 minutes, eliminating open-heart surgery.^[18]

In development are stents with biocompatible surface coatings which do not elute drugs, and also absorbable stents (metal or polymer).

References

1. ^¹{{Cite book|url=https://www.worldcat.org/oclc/1021152059|title=Braunwald's heart disease : a textbook of cardiovascular medicine|others=Zipes, Douglas P.,, Libby, Peter,, Bonow, Robert O.,, Mann, Douglas L.,, Tomaselli, Gordon F.,, Braunwald, Eugene, 1929-|isbn=9780323555937|edition= Eleventh |location=Philadelphia, PA|oclc=1021152059}}
2. ^{{cite journal |doi=10.1093/eurheartj/ehl088 |title=A comparison of pharmacologic therapy with/without timely coronary intervention vs. primary percutaneous intervention early after ST-elevation myocardial infarction: the WEST (Which Early ST-elevation myocardial infarction Therapy) study |author1=Armstrong P |author2=WEST Steering Committee |journal=Eur Heart J |year=2006 |volume=27 |issue=10 |pages=1530–1538 |pmid=16757491}}
3. ^{{Cite book|url=https://www.worldcat.org/oclc/994570810|title=Goodman & Gilman's the pharmacological basis of therapeutics|others=Brunton, Laurence L.,, Knollmann, Björn C.,, Hilal-Dandan, Randa,|isbn=9781259584732|edition= Thirteenth |location=[New York]|oclc=994570810}}
4. ^Intravascular Ultrasound - Angioplasty.Org
5. ^{{cite journal |doi=10.1016/j.ahj.2005.01.050 |url=http://www.medscape.com/viewarticle/517637 |journal=Am Heart J |date=November 2005 |volume=150 |issue=5 |pages=994–9 |title="Full metal jacket" (stented length > or =64 mm) using drug-eluting stents for de novo coronary artery lesions |vauthors=Aoki J, ((Ong ATL)), ((Granillo GAR)), McFadden EP, ((van Mieghem CAG)), Valgimigli M, Tsuchida K, Sianos G, Regar E, ((de Jaegere PPT)), van der Giessen WJ, de Feyter PJ, van Domburg RT, Serruys PW |pmid=16290984}}
6. ^Angioplasty 101 Angioplasty.Org
7. ^{{cite web |url=http://indianheartjournal.com/ihj06/mar_apr_06/108-119.html |title=Archived copy |accessdate=2010-09-28 |deadurl=yes |archiveurl=https://web.archive.org/web/20101205122603/http://indianheartjournal.com/ihj06/mar_apr_06/108-119.html |archivedate=2010-12-05 |df= }}
8. ^{{Cite web|url=https://www.nhlbi.nih.gov/health-topics/stents|title=Stents {{!}} National Heart, Lung, and Blood Institute (NHLBI)|website=www.nhlbi.nih.gov|language=en|access-date=2018-11-01}}
9. ^{{cite book | last = Michel | first = Thomas | editor = Laurence L. Brunton | editor2 = John S. Lazo | editor3 = Keith L. Parker | title = Goodman & Gilman's The Pharmacological Basis of Therapeutics | origyear = 1941 | edition = 11th | year = 2006 | publisher = McGraw-Hill | location = New York | pages = 842 | chapter = Treatment of Myocardial Ischemia}}
10. ^¹Kolata, Gina. [https://www.nytimes.com/2004/03/21/us/new-heart-studies-question-the-value-of-opening-arteries.html "New Heart Studies Question the Value Of Opening Arteries"] The New York Times, March 21, 2004. Retrieved January 14, 2011.
11. ^{{cite news |url=https://www.bloomberg.com/news/2013-10-24/the-cardiologist-who-spread-heart-disease.html |title=The Cardiologist Who Spread Heart Disease |work=Bloomberg|author=David Armstrong |date= 24 October 2013}}
12. ^{{cite news|url=https://www.bloomberg.com/news/2013-09-26/deaths-linked-to-cardiac-stents-rise-as-overuse-seen.html |title=Deaths Linked to Cardiac Stents Rise as Overuse Seen |author=Peter Waldman |author2=David Armstrong |author3=Sydney P. Freedberg |last-author-amp=yes |date= 26 September 2013 |work=Bloomberg}}
13. ^[https://www.wsj.com/articles/SB20001424052748703652104574652401818092212 A simple health care fix fizzles out], Kenneth J. Winstein, Wall Street Journal, Feb. 11, 2010.
14. ^{{cite journal |doi=10.1056/NEJMoa070829 |title=Optimal medical therapy with or without PCI for stable coronary disease |author1=Boden WE |author2=O'Rourke RA |author3=Teo KK |author4=Hartigan PM |author5=Maron DJ |author6=Kostuk WJ |author7=Knudtson M |author8=Dada M |author9=Casperson P |author10=Harris CL |author11=Chaitman BR |author12=Shaw L |author13=Gosselin G |author14=Nawaz S |author15=Title LM |author16=Gau G |author17=Blaustein AS |author18=Booth DC |author19=Bates ER |author20=Spertus JA |author21=Berman DS |author22=Mancini GB |author23=Weintraub WS |author24=COURAGE Trial Research Group |journal=N Engl J Med |date=2007-04-12 |volume=356 |issue=15 |pages=1503–16 |pmid= 17387127 }}
15. ^{{cite journal |doi=10.1016/j.jacc.2003.08.065 |title=The medicine, angioplasty, or surgery study (MASS-II): a randomized, controlled clinical trial of three therapeutic strategies for multivessel coronary artery disease: one-year results |vauthors=Hueb W, Soares PR, Gersh BJ, César LA, Luz PL, Puig LB, Martinez EM, Oliveira SA, Ramires JA |journal=J Am Coll Cardiol |date=2004-05-19 |volume=43 |issue=10 |pages=1743–51 |pmid=15145093}}
16. ^http://circ.ahajournals.org/cgi/content/abstract/circulationaha;115/9/1082 MASS-II 5yr follow-up.
17. ^{{ClinicalTrialsGov|NCT00114972}} SYNTAX trial 2005-2008
18. ^https://www.google.com/patents/US3657744