Adverse Drug Events: A Focus on Anticoagulation Steve Meisel, Pharm.D., CPPS Director of Patient Safety Fairview Health Services, Minneapolis, MN

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Adverse Drug Events: A Focus on Anticoagulation Steve Meisel, Pharm.D., CPPS Director of Patient Safety Fairview Health Services, Minneapolis, MN

Fairview Health Services 6 hospitals, ranging from rural to academic 50+ primary care clinics Home care/hospice, home infusion, long term care, retail pharmacy, PBM 20,000 employees, 3,000 physicians 73,000 annual admissions; 175,000 ED visits; 1 million clinic visits $3 billion gross revenue > 8,000,000 annual inpatient doses dispensed 1.7 million annual retail pharmacy prescriptions

Disclaimer

What is medication safety?

What is medication safety? Absence of errors Absence of adverse events as measured by? Absence of preventable adverse events Absence of reportable events Adherence to guidelines/standards Adherence to NPSG Positive cultural surveys Good responses to self-assessment surveys (ISMP, Leapfrog)?

What is safety? Safety is a condition defined by the perception of the customer (patient). Safety is not synonymous with the absence of risk or adverse events. Instead it is marked by the knowledge and comfort that all efforts are being made to prevent everything we know how to prevent and that we are striving to make things even better. Aviation, automobile, nuclear power Error reduction, adherence to guidelines, etc are tactics, not strategies

Harm vs. Error

Fairview s ADE Measurement System 100% real-time review of triggers for harm from high hazard drugs: Naloxone use (narcotics) Flumazenil use (sedatives) Blood sugar <40 mg/dl (antidiabetic agents) INR >5 (warfarin)* PTT >200; anti-xa level > 1.6 (heparin) prothrombin complex concentrate and coagulation factor VIIa (rivaroxaban and dabigatran) * Threshold of 6 until 2Q 2012

Anticoagulation Review Criteria A legitimate screen. Example: a bedside PTT reading of 215 seconds but a subsequent laboratory analysis was 135 seconds. In these cases, the record is coded as artifact and no further action would be taken. If the screen is determined to be legitimate, was it associated with an anti-coagulant? Example: An INR of 7 relating to liver disease or malnutrition. In these cases, the record is coded as no adverse drug event.

Anticoagulation Review Criteria If the high INR or PTT or antidote was associated with the use of an anticoagulant and there was clinical intervention, an ADE has occurred. Simply modifying or holding the dose is NOT a clinical intervention The use of an antidote automatically mean that an adverse event occurred. Exception: planned reversals such as prior to surgery Warfarin-related bleeding resulting from outpatient services do NOT count as an ADE it is related to a prior hospital discharge.

Anticoagulation Harm Ratings

ADE Gap Analysis Anticoagulants Courtesy of the Minnesota Hospital Association Hospital Engagement Network

1. Antithrombotic management practices 1a) Responsibility is assigned for coordinating anticoagulation monitoring functions. A process exists to ensure fields contained in standard protocols/order sets/ flowsheets are consistently populated (manually or automatically) with key information, including at a minimum: 1b) The patient s diagnosis 1c) Allergies 1d) Most recent pertinent laboratory results

1. Antithrombotic management practices Standard policies & practices exist for managing the initiation and maintenance of anticoagulation therapy which include: 1e) The specific medication used (e.g., low molecular weight heparin (LMWH), warfarin, unfractionated heparin (UFH), Vitamin K reversal, direct thrombin inhibitors) 1f) The condition being treated 1g) The potential for drug interactions

1. Antithrombotic management practices 1h) A protocol exists to determine the need to reverse supratherapeutic INR values based on key criteria, (e.g., the INR value, the presence or absence of bleeding, individual patient situation, e.g., imminent surgery). 1i) A process exists to ensure that anti-platelet agents are used for the appropriate indication (e.g., patients with mechanical valves, acute coronary syndrome or recent stent or bypass surgery.)

1. Antithrombotic management practices Vitamin K practice specifies (in patients with no evidence of warfarin associated bleeding): 1j) No routine use of Vitamin K for INR between 4.5 10. 1k) The use of oral Vitamin K for INR >10. In patients with warfarin associated major bleeding: 1l) Reversal may be accomplished with the addition of Vitamin K 5-10 mg given slow IV infusion. 1m) Reversal may also be accomplished with prothrombin complex concentrate and the addition of Vitamin K 5-10 mg given slow IV infusion.

2. Prevention & mitigation practices (all) 2a) Antithrombotics are included in the defined list of high alert medications. 2b) Practitioners are alerted to significant drug interactions for patients on antithrombotic agents. 2c) Prescribers are reminded to evaluate the need for antithrombotic therapy when antithrombotics are being held for future surgical purposes. 2d) A pharmacy managed system exists for antithrombotic drug shortage situations which outlines how standard medication safety processes will be followed.

2. Prevention & mitigation practices (all) 2e) IV antithrombotic orders cannot be entered into the pharmacy and order entry systems without including patient weight. Smart infusion pumps are used for the IV administration of all antithrombotics (including platelet inhibitors), with functionality employed to: 2f) Intercept and prevent wrong dose errors. 2g) Intercept and prevent wrong infusion rate errors.

3. Therapeutic practices (all) A process exists, using a standardized tool, to address and document the following prior to initiating antithrombotic therapy: 3a) Nutritional status 3b) Recent trauma 3c) Surgery 3d) Bleeding problems experienced while receiving any previous antithrombotic therapy 3e) Clotting history 3f) Drug/drug interactions 3g) Pharmacists assist with identification of alternative antithrombotic agents when contraindications exist.

3. Therapeutic practices (all) 3h) The indication and therapeutic goal for antithrombotic therapy is documented in the medical record and communicated to pharmacy for monitoring and managing patient therapy. Processes exists for timely access to routine test results which include: 3i) INR, PTT and anti-xa level available within 2 hours. 3j) Health care providers can readily access inpatient and outpatient laboratory results to guide antithrombotic therapy. 3k) When an antithrombotic agent is administered in the ED or other outpatient settings (e.g., cardiac cath lab, radiology), the inpatient medication record and chart is updated to communicate this information to other practitioners.

3. Therapeutic practices (all) For critical test results reporting, the facility has defined acceptable lengths of time between: 3l) Ordering critical hematologic tests (e.g., INR, PPT) and reporting of the test results. 3m) The availability of the results and confirmation of receipt by a health care provider. 3n) The receipt of results by a health care provider and clinically appropriate antithrombotic dose changes

4, Warfarin management practices Standard processes exist for initiation of warfarin therapy and daily dosing, which include: 4a) Collection of baseline lab values prior to prescribing anticoagulant. (e.g. warfarin-naïve patient (30 days prior), warfarin maintenance patient (24 hr prior). 4b) The INR is the primary laboratory test used to monitor and adjust warfarin therapy. 4c) Nutritional assessment 4d) Drug/drug interactions 4e) Lab values 4f) History of thrombosis or bleeding event 4g) Recent trauma or surgery

4, Warfarin management practices 4h) Ability to adjust INR target range for clinical indication. 4i) Screening for interactions between enteral nutrition products and antithrombotic therapy. (e.g., drug/tube feed interactions.) 4j) Obtaining blood draws for INR at the same time each day. 4k) Administering warfarin at the same time each day after INR results are available (e.g., afternoon / evening) 4l) Warfarin is started on Day 1 or 2 of LMWH or UFH therapy initiation.

4, Warfarin management practices 4m) Pharmacists can automatically modify warfarin therapy doses or directly contact the prescriber when laboratory values are below or above approved target ranges. 4n) When warfarin therapy is initiated for a patient with active thrombosis, heparin or LMWH is continued until warfarin has been administered for a minimum of 5 (five) days and the INR reaches a therapeutic level for 2 (two) consecutive days. 4o) A process exists for detection of contraindication of warfarin in pregnancy.

5. Warfarin prevention & mitigation practices Warfarin management practices include: 5a) Notification of dietary services when a patient is receiving warfarin therapy. 5b) Automatic nutrition consults when patients are first placed on warfarin to avoid drug-food interactions 5c) Warfarin is dispensed in unit dose only (e.g., warfarin tablets are not split). 5d) Warfarin is not available as floor stock unless stored in an automated dispensing cabinet that is interfaced with pharmacy. 5e) All strengths of warfarin tablets dispensed within the facility are purchased from a single manufacturer.

5. Warfarin prevention & mitigation practices The facility s practice for handoff communication to the next provider of care includes: 5f) Inpatient warfarin dosing history 5g) Inpatient INR value history 5h) Date the next INR is due 5i) Daily warfarin dosing schedule to be followed until date of next INR 5j) A confirmed appointment scheduled for laboratory, physician, and/or antithrombotic clinic

5. Warfarin prevention & mitigation practices The facility s practice for patients who are being discharged on warfarin therapy and have a subtherapeutic INR includes a transition plan for: 5k) Consistent evaluation regarding the need for LMWH until a therapeutic INR is reached 5l) Maintaining patient on LMWH until a therapeutic INR is reached, (when appropriate)

6) Parenteral anticoagulant management practices Processes are in place for: 6a) Safely managing the care & removal of epidural catheters placed during regional anesthesia when LMWH has been administered. 6b) Monitoring and/or discontinuing antithrombotic therapy prior to invasive procedures. (e.g., INR within specific range or target.) 6c) Only continuous infusions are used for therapeutic IV heparin (no intermittent IV administration). 6d) When LMWH or UFH therapy is greater than 3 days, a process exists that ensures that a platelet count and serum creatinine are repeated every 3 days.

6) Parenteral anticoagulant management practices 6e) Standard guidelines are used for laboratory monitoring of LMWH in special populations (e.g. renal dosing, pregnancy, and morbid obesity) When laboratory reagents that are used to measure the PTT or other hematological tests are changed a process exists to: 6f) Inform prescribers, pharmacists and nurses about the change. 6g) Update affected dosing protocols and order sets.

7) Parenteral anticoagulant prevention & mitigation strategies Processes exist to eliminate errors in preparation, storage, and dispensing which includes: 7a) Utilizing unit dose LMWH (round to the nearest dose if using a pen) 7b) Limiting concentrations of Heparin stored in automated dispensing machines and as floor stock (e.g., Do not store 10,000 units/ml 1mL vials) Dispensing commercially prepared, pre-mixed IV solutions of UFH: 7c) In limited concentrations. 7d) In limited vial sizes. 7e) In prefilled heparin flush syringes.

7) Parenteral anticoagulant prevention & mitigation strategies Independent double-check for UFH are used (e.g., with smart pump technology and/or nurse doublecheck) with: 7f) Each new bag hung 7g) Each rate change

8) Parenteral anticoagulant therapeutic strategies Processes exist to initiate and monitor heparin via lab values including: 8a) A baseline hemoglobin, hematocrit, serum creatinine and platelet count are obtained prior to initiating antithrombotic therapy with UFH or LMWH. 8b) PTTs are obtained no sooner than 6-8 hours after UFH initiation. 8c) Laboratory tests have standard intervals for assessment. (e.g., hgb every 3 days, platelets every 3 days.) 8d) Prior to ordering any heparin product, prescribers are required to specifically ask patients if they have a known history of heparin induced thrombocytopenia (HIT) and/or an allergy to heparin; and positive responses are documented in the medical record.

8) Parenteral anticoagulant therapeutic strategies 8e) A VTE prophylaxis protocol exists and is used for acutely ill or critically ill medical patients that includes use of low dose UFH, LMWH or fondaparinux. 8f) The renal dosing program allows a pharmacist or prescriber to routinely adjust the doses of LMWH, Factor Xa inhibitors, and direct thrombin inhibitors. 8g) The documentation process for LMWH injections includes date and time of dose, and site of injection. For patients on UFH: 8h) If platelet count decreases to less than 100,000/mm 3 or less than 50% of the baseline that the patient is evaluated for HIT in real-time. 8i) If the patient is diagnosed with HIT, all sources of heparin are discontinued including heparin flush.

9) Implement appropriate critical thinking and knowledge strategies Interdisciplinary education on antithrombotic therapy is provided and includes: 9a) Initial training for new hires and existing staff, including protocols and guidelines. 9b) Post test incorporating a case-study approach to demonstrate proficiency. 9c) Plan for targeting gaps in knowledge. 9d) Ongoing antithrombotic education is provided to direct care staff when new relevant information is available.

10) Provide patient and family education 10a) When initiating therapy, patients/caregivers receive verbal & written information on purpose, action, side effects, & monitoring. Processes exist to educate patients & families, using teach-back method, to ensure safe therapy including: 10b) Indication 10c) Symptoms for monitoring 10d) Dietary issues 10e) Drug interactions 10f) Disease interactions 10g) Monitoring requirements 10h) Duration of therapy 10i) Potential adverse effects 10j) Pharmacists are available for consultations to assist with patient

Questions and Discussion