Complications After Dental Sedation: A Myotonic Mystery Case Report

Author:

Karamlou Milad1,Asaria Iman2,Barron Jaime2,Boutros Petra2,Fisher Vincent2,Grandinetti Rachel2,Johnson Julian2,Richard Emily2,Susko David2,Urrutia Cristobal2,Woolsey Bryce3,Baumann Ronald4,Cottle James5,Sweaney Richard5,Wenzel Mark6,Nusstein John7,Hall David8

Affiliation:

1. *Former Resident, The Ohio State University College of Dentistry General Practice Residency Program, Columbus, Ohio

2. †Resident, The Ohio State University College of Dentistry General Practice Residency Program, Columbus, Ohio

3. ‡Chief Resident, The Ohio State University College of Dentistry General Practice Residency Program, Columbus, Ohio

4. §Former Assistant Professor and Attending, The Ohio State University College of Dentistry General Practice Residency Program, Columbus, Ohio,

5. ||Assistant Professor and Attending, The Ohio State University College of Dentistry General Practice Residency Program, Columbus, Ohio

6. #Program Director and Hospital Attending, The Ohio State University College of Dentistry General Practice Residency Program and Wexner Medical Center, Columbus, Ohio

7. **Professor and Chair Division of Endodontics, The Ohio State University College of Dentistry, Columbus, Ohio

8. ††Associate Professor and Hospital Attending, The Ohio State University College of Dentistry General Practice Residency Program and Wexner Medical Center, Columbus, Ohio

Abstract

Myotonic dystrophy (dystrophia myotonica; DM) is an uncommon progressive hereditary muscle disorder that can present with variable severity at birth, in early childhood, or most commonly as an adult. Patients with DM, especially type 1 (DM1), are extremely sensitive to the respiratory depressant effects of sedative-hypnotics, anxiolytics, and opioid agonists. This case report describes a 37-year-old male patient with previously undiagnosed DM1 who received dental care under minimal sedation using intravenous midazolam. During the case, the patient experienced 2 brief episodes of hypoxemia, the second of which required emergency intubation after propofol and succinylcholine and resulted in extended hospital admission. A lipid emulsion (Liposyn II 20%) infusion was given approximately 2 hours after the last local anesthetic injection due to slight ST elevation and suspicion of local anesthetic toxicity (LAST). Months after treatment, the patient suffered a fall resulting in a fatal traumatic brain injury. Complications noted in this case report were primarily attributed to the unknown diagnosis of DM1, although additional precipitating factors were likely present. This report also provides a basic review of the literature and clinical guidelines for managing myotonic dystrophy patients for dental care with local anesthesia, sedation, or general anesthesia.

Publisher

American Dental Society of Anesthesiology (ADSA)

Subject

Anesthesiology and Pain Medicine

Reference29 articles.

1. National Institutes of Health. Myotonic dystrophy. Updated August 21, 2017. https://rarediseases.info.nih.gov/diseases/10419/myotonic-dystrophy

2. Hines RL, Marschall KE, eds. Skin and musculoskeletal diseases. In:Handbook for Stoelting's Anesthesia and Co-Existing Disease. 4th ed. Philadelphia, PA: Elsevier/Saunders;2013: 270– 287.

3. Campbell N, Brandon B, Day JW, Moxley R. Practical suggestions for the anesthetic management of a myotonic dystrophy patient. In:Myotonic Dystrophy Foundation Toolkit. Oakland, CA: Myotonic Dystrophy Foundation;2015; 73– 80.

4. Russell S, Anaesthesia Hirsch N. and myotonia. Br J Anaesth. 1994; 72: 210– 216.

5. Veyckemans F, Scholtes JL. Myotonic dystrophies type 1 and 2: anesthetic care. Pediatr Anesth. 2013; 23: 794– 803.

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