Pacemaker Related Infective Endocarditis from Staphylococcus Lugdunensis: A Case Report

Staphylococcus lugdunensis is a common skin flora not typically associated with infection. There are, however, several cases reported in the literature of Staphylococcus lugdunensis as a causative bacterium of various infections. This paper reports an additional case of pacemaker associated endocarditis with Staphylococcus lugdunensis as the causative bacterium.


Introduction
Staphylococcus lugdunensis is a common skin �ora that is seldom a causative organism of infection. It is a coagulasenegative staphylococcus that was �rst described in 1988 and has been associated with various community and nosocomial infections including native/prosthetic valve endocarditis, skin and so tissue infections, catheter-related infections, ventriculoperitoneal shunt infections, prosthetic joint infections, and pacemaker related infections [1][2][3][4]. S. lugdunensis is proving to be more virulent than other coagulase-negative staphylococci, which is thought to be related to several of its unique abilities including the production of a toxin-like hemolytic peptide, adhesion promoting molecules, various en�ymes, and bio�lm formation [2]. It also produces a Von Willebrand bound binding protein that allows it to adhere to the endocardium endothelium lesions [2]. e frequency of S. lugdunnsis is likely underreported because it is easily confused with S. aureus through S. lugdunnsis' ability to produce clumping factors and the fact that many labs do not further isolate out coagulase-negative staphylococci variants [2]. Fortunately, it is oen susceptible to most antibiotics already used to treat other staphylococcal infections with little reported resistance. An estimated 25% of strains are capable of producing b-lactamase and even methicillin resistance is rarely reported [2].

Case
A 74-year-old Caucasian female presents to the emergency department of a local community hospital with a chief complaint of diarrhea for the past 3-4 days and a productive cough. All other review of systems was documented as negative. Her medical history was positive for hypertension, TIA, and an unspeci�ed cardiac condition requiring a pacemaker. Her home medications included Bumetanide, digoxin, atorvastatin, carvedilol, lisinopril, and oral potassium supplement. Surgical and social histories were noncontributory. All history was obtained from the patient who was reported as alert and oriented for the duration of the emergency room stay.
On initial presentation, her vital signs were as follows: a blood pressure of 131/84, pulse of 108, respiratory rate of 20, temperature of 38.6, and a pulse oximetry of 94% on room air.
She was reported to be in a new onset atrial �brillation with a rapid ventricular rate. e rest of her examination was positive for the tachycardia with an irregularly irregular rhythm and 2+ pitting edema bilaterally in her lower extremities.
Overall, this patient presented with a new onset atrial �brillation with a rapid ventricular rate, acute anemia without signs of active bleeding, non-ST segment elevation myocardial infarction (NSTEMI), acute renal failure, and an elevated bilirubin and INR. Suspected etiology was initially hypovolemia from sepsis confounded by further volume loss via diarrhea. An abdominal ultrasound was performed and was negative for acute pathology. Blood and stool cultures were obtained and a stool for Clostridium difficile was negative.
Treatment in the emergency department consisted of �uid resuscitation with 0.9% normal saline (NS) boluses, for a total of 3L of NS in the emergency department as well as 2 units of packed red blood cells were transfused. She received 2 liters of oxygen via nasal cannula and was given 1 gram of intravenous ceriaxone for UTI. Her four-hour repeat troponin was elevated to 1.97 ng/ml (<0.10 ng/ml) and the lactic acid elevated to 6.0 mmol/L (0.4-1.8 mmol/L). yroid studies were ordered and not found to be a contributing factor to the new atrial �brillation with rapid ventricular rate with a thyroid stimulating hormone (TSH) of 5.72 uIU/ml (0.35-5.50 uIU/ml) and free T4 of 0.88 ng/dL (0.59-1.17 ng/dL). She remained in the emergency department approximately �ve hours before a bed was available in the step-down intensive care unit.
e antibiotics were switched to intravenous cefepime 2 grams every eight hours, 250 mg of oral vancomycin every eight hours, and 500 mg of intravenous metronidazole every eight hours on the �oor. She was seen by cardiology, nephrology, gastroenterology, hematology, and infectious disease specialists. General surgery was consulted for possible abdominal etiology of sepsis per documentation. CT abdomen without contrast revealed a low density lesion within the spleen, mesenteric edema, questionable bowel wall thickening of the ascending colon, and a right pleural effusion with bilateral patchy consolidations. General surgery opted to continue antibiotics at that time without immediate surgical intervention.
Labs were repeated the following morning. Her lactate had elevated to 11.2 mmol/dL (0.4-1.8 mmol/L) despite resuscitation. e leukocytosis elevated to 17.4 K/uL (3.8-10.6 K/uL), potassium to 5.4 mmol/L (3.5-5.0 mmol/L), bicarbonate of 7 mmol/L (24-32 mmol/L) with anion gap of 23 (8-16). Troponin I elevated to 2.88 ng/ml (<0.10 ng/ml), Cr. to 2.3 mg/dL (0.6-1.2 mg/dL), and INR >19.2 (0.80-1.20). e patient had developed disseminated intravascular coagulation (DIC), likely secondary to sepsis. Transfusion of four units of fresh frozen plasma and six units of platelets were initiated. Hydrocortisone 25 mg intravenously every 6 hours and intravenous Vitamin K 10 mg were administered. e patient ultimately went into acute respiratory failure from the �uids and blood products she received, was intubated by anesthesia, and moved to the intensive care unit. She also became hypotensive and required a continuous infusion of norepinephrine, subsequently developed oliguria, and a right femoral dialysis catheter was placed in case she would later require dialysis. Her blood cultures came back positive for gram positive cocci identi�ed as Staphylococcus lugdunensis. Infectious endocarditis was suspected and nafcillin was started. A transthoracic 2D echo was performed and showed large vegetation on the posterior lea�et of the mitral valve. Transesophageal echocardiogram con�rmed this �nding and further identi�ed additional vegetation on the anterior lea�et of the mitral valve measuring 0.4 cm. e posterior vegetation measured 1.8 cm and was noted to be very mobile. At this point, the CT �ndings were thought to be secondary to septic emboli. e laboratory abnormalities began to improve the following day and she was started on rifampin in addition to the nafcillin with all other antibiotics discontinued. Her leukocytosis, lactate, troponin, and creatinine began to trend down, but the decision was made to transfer the patient to a local tertiary center a�liate for the de�nitive care of pacemaker removal where she was accepted to the medical intensive care unit. e patient had a 24-day course between the two facilities. Her DIC resolved and she was still in the atrial �brillation with a controlled ventricular rate during her stay. On hospital day 10, the pacemaker and its leads were removed out of concern, it was the source of infection. It was reported to be implanted on 1/15/2010 and was a Biotronik Cyclos DR with one lead in the right atrium and another in the right ventricle. e leads were sent to lab for tip cultures. e right atrial lead showed rare S. lugdunensis, while the right ventricle lead revealed few S. lugdunensis that was susceptible to nafcillin. A temporary transvenous pacemaker was immediately replaced; however, this pacemaker was found not necessary and subsequently removed 48 hours later. e patient was still on intravenous na�cillin and rifampin and was �nally extubated on hospital day 11. Repeat blood cultures were negative for growth aer 5 days on hospital days 11, 19, and 20. e discharge summary reported that the nafcillin was discontinued because she began to develop rashes. She was discharged on oral warfarin for her atrial �brillation. Her kidney function returned to baseline with creatinine of 1.2 mg/dL (0.6-1.2 mg/dL). Subsequent transthoracic echo cardiograms revealed that the mitral valve vegetations were improving. She was discharged to a sub-acute rehab facility with continued intravenous nafcillin therapy and outpatient followup with cardiology and infectious disease.
e patient returned to the original community hospital's emergency department three days aer discharge with chief complaint of mental status changes. She was found to have bright red blood per rectum and an anemia of 6.0 g/dL (12.0-15.0 g/dL) with a hemoglobin level of 9.0 g/dL (12.0-15.0 g/dL) reported from the tertiary facility at discharge. e decision was made by family to make the patient not to resuscitate (DNR) status with no desired intubation or mechanical ventilation. e patient was only oriented to person at this time and incapable of making her own medical decisions. She was placed in hospice care and expired two days later.

Discussion
S. lugdunensis is as emerging as a pathogen that presents similar to S. aureus. It has been associated with several cases of infective endocarditis with an inclination for le sided, native valve related infections [5]. Despite its reported high levels of susceptibility to various antibiotics, medical treatment alone is oen unsuccessful and surgical interventions are oen required. Jung et al. report an increase in mortality by 3.1 times if native valve endocarditis is treated medically alone without surgical intervention if S. lugdunensis is the causative agent [6].
is case presents an additional presentation of pacemaker associated endocarditis with S. lugdunensis as the causative agent. One article cites 100 cases of endocarditis secondary to S. lugdunensis [7] with another 7 cases of pacemaker associated infective endocarditis from S. lugdunensis between 1990 and 2003, four of which were found through the literature review and three within their institutions [1]. S. lugdunensis is proving to be a considerable pathogen once introduced into the body with increased virulence compared to other coagulase-negative staphylococci. It will be increasingly important to isolate out different species of the coagulase-negative staphylococci found to be causing systemic infections to further track and identify S. lugdunensis and its clinical characteristics.