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What is InpharmD™?


Literature searching is tedious. InpharmD™ is here to help.

Clinical pharmacists can ask any question, anytime, from anywhere, and we’ll perform a custom literature search.

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This is how InpharmD™ transforms LITERATURE.

What's Being Asked...

What evidence is available regarding the use of dantrolene for malignant hyperthermia?
what happens if you administer pregablin with a patient with low creatinine clearance
What evidence is available regarding the use of rituximab in CNS vasculitis?
Are doses greater than 60 mg for Cymbalta no more effective for MDD or GAD?
Can enoxaparin be used for DVT prophylaxis in a patient on hemodialysis?

What would you like to ask InpharmD™?

InpharmD's Answer GPT's Answer

Author:Rachel Deryck, PharmD, BCPS + InpharmD™ AI

INTRODUCTION BY INPHARMD™ RESEARCHER

Dantrolene is the only medication known to specifically treat malignant hyperthermia (MH) and is recommended for use by various societal guidelines. Notably, no preferences are provided regarding dantrolene formulations for MH reversal (i.e., Dantrium®, Revonto®, and Ryanodex®). While guideline-recommended dosing regimens for intravenous dantrolene may vary, shortened time-to-administration windows following confirmed or suspected MH are heavily emphasized as a key factor that impacts patient...

According to the Japanese Society of Anesthesiologists (JSA), malignant hyperthermia (MH) develops in one to two patients in every 100,000 general anesthesia cases. Prevalence in males is more common at a 3:1 ratio in comparison to females. Mortality has been less than 10% since the year 2000 in patients treated with dantrolene. Treatment with dantrolene is recommended, and it should be administered immediately if symptoms of MH are suspected. Evidence suggests dantrolene ≥1 mg/kg is necessary to resolve muscle rigidity and prevent recurrence, and the JSA guidelines recommend 2 mg/kg over 15 minutes through a large-bore intravenous (IV) line. Doses may be repeated and adjusted up to a maximum of 7 mg/kg until the patient’s condition improves. [1] Per European Malignant Hyperthermia Group guidelines on the management of malignant hyperthermia crisis, it is recommended to give dantrolene at a dose of 2-2.5 mg/kg IV. The dose of dantrolene should be based on the patient’s actual bod...

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A search of the published medical literature revealed 2 studies investigating the researchable question:

What evidence is available regarding the use of dantrolene for malignant hyperthermia?

Level of evidence
D - Case reports or unreliable data  

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[1] JSA guideline for the management of malignant hyperthermia crisis 2016. J Anesth. 2017;31(2):307-317.
[2] Glahn KPE, Girard T, Hellblom A, et al. Recognition and management of a malignant hyperthermia crisis: updated 2024 guideline from the European Malignant Hyperthermia Group. Br J Anaesth. 2025;134(1):221-223. doi:10.1016/j.bja.2024.09.022
[3] Hopkins PM, Girard T, Dalay S, et al. Malignant hyperthermia 2020: Guideline from the Association of Anaesthetists. Anaesthesia. 2021;76(5):655-664. doi:10.1111/anae.15317
[4] Carlson B, Wormuth L. Malignant Hyperthermia: An Overview. US Pha...

InpharmD's Answer GPT's Answer

Author:Neil Patel, PharmD, BCPS + InpharmD™ AI

INTRODUCTION BY INPHARMD™ RESEARCHER

Studies show gabapentinoids given to patients with renal impairment can result in altered mental status and falls if administered without dose adjustment.

Gabapentin and pregabalin exhibit unique pharmacokinetic properties that pose challenges in achieving therapeutic concentrations, especially in patients with renal impairment. Neither drug undergoes hepatic metabolism; instead, they are primarily excreted unchanged through the urine, minimizing the risk of hepatic cytochrome P450-related drug-drug and drug-food interactions. Gabapentin's clearance is linearly correlated with creatinine clearance (CrCl) and may involve active tubular secretion via organic cation transporter-1 (OCT-1), though this is not fully clinically significant due to its primary filtration excretion. Pregabalin undergoes some tubular reabsorption, with a clearance rate lower than that of gabapentin. Both drugs require dose adjustments based on the degree of renal impairment. For instance, pregabalin maximum recommended dosages are altered based on CrCl values: 100 mg TID or 150 mg BID for CrCl 30-59 mL/min, 50 mg TID or 75 mg BID for CrCl 15-29 mL/min, 75 mg onc...

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A search of the published medical literature revealed 2 studies investigating the researchable question:

What happens if you administer pregablin with a patient with low creatinine clearance?

Level of evidence
C - Multiple studies with limitations or conflicting results  

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[1] Raouf M, Atkinson TJ, Crumb MW, Fudin J. Rational dosing of gabapentin and pregabalin in chronic kidney disease. J Pain Res. 2017;10:275-278. Published 2017 Jan 27. doi:10.2147/JPR.S130942
[2] Ishida JH, McCulloch CE, Steinman MA, Grimes BA, Johansen KL. Gabapentin and Pregabalin Use and Association with Adverse Outcomes among Hemodialysis Patients. J Am Soc Nephrol. 2018;29(7):1970-1978. doi:10.1681/ASN.2018010096

InpharmD's Answer GPT's Answer

Author:Dylan Brown, PharmD, BCPS + InpharmD™ AI

INTRODUCTION BY INPHARMD™ RESEARCHER

The majority of data is focused on rituximab as a combination regimen for ANCA-associated vasculitis, which is generally considered to be effective and beneficial for consideration as remission therapy compared to other immunosuppressive therapy. Data specific to CNS vasculitis is more limited to patient cases or retrospective reviews, but similarly suggest that rituximab may also facilitate remission of symptoms.

Rituximab, a CD20-directed cytolytic antibody, is indicated for both induction and maintenance therapy in two subtypes (granulomatosis with polyangiitis, GPA; microscopic polyangiitis, MPA) of ANCA-associated vasculitis (AAV). The 2020 expert consensus guidelines from the British Society for Rheumatology were developed in order to provide in-depth clinical guidance for rituximab’s use as a remission maintenance therapy. The guidelines suggest that for new and relapsing patients with GPA/MPA, rituximab is recommended for the maintenance of remission following successful rituximab or cyclophosphamide induction. The same recommendation applies for eosinophilic granulomatosis with polyangiitis (EGPA), the third subtype of AAV, despite limited evidence related to this relatively understudied phenotype of AAV. The guidelines state that the treatment response to rituximab in EGPA patients may differ, and steroidal cessation may present more challenges. [1] The expert panel recommends fi...

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A search of the published medical literature revealed 7 studies investigating the researchable question:

What evidence is available regarding the use of rituximab in CNS vasculitis?

Level of evidence
C - Multiple studies with limitations or conflicting results  

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[1] Tieu J, Smith R, Basu N, et al. Rituximab for maintenance of remission in ANCA-associated vasculitis: expert consensus guidelines. Rheumatology (Oxford). 2020;59(4):e24-e32. doi: 10.1093/rheumatology/kez640
[2] Emmi G, Bettiol A, Gelain E, et al. Evidence-Based Guideline for the diagnosis and management of eosinophilic granulomatosis with polyangiitis. Nat Rev Rheumatol. 2023;19(6):378-393. doi:10.1038/s41584-023-00958-w
[3] Dutertre M, Pugnet G, de Moreuil C, et al. 0854 Long-term Efficacy of Remission-induction Regimens for Eosinophilic Granulomatosis with Polyangiitis. ACR Converge...

InpharmD's Answer GPT's Answer

Author:Kevin Shin, PharmD, BCPS + InpharmD™ AI

INTRODUCTION BY INPHARMD™ RESEARCHER

Duloxetine has demonstrated efficacy in both older adults and pediatric patients using flexible dosing regimens ranging from 30 to 120 mg daily. In older adults, symptom improvement was observed across various dose levels, with some benefiting from doses above 60 mg daily. Pediatric studies suggest that doses of 60 mg or higher are often needed for clinical effect, though findings on efficacy have been mixed. Across both populations, the safety profile was consistent, with common adverse effe...

Two double-blind, randomized controlled trials investigated the efficacy and safety of duloxetine at 60 mg and 120 mg daily doses in patients with major depressive disorder (MDD). The first study focused on nonremitters and remitters after initial 6-week treatment, while the second study examined severely depressed hospitalized patients. In both trials, researchers found no significant clinical advantages of the 120 mg dose over the 60 mg dose. The first study revealed that nonremitters randomly reassigned to either 60 mg or 120 mg achieved similar remission rates (approximately 30%), with 85.5% of initial remitters maintaining their improvement. The second study, involving hospitalized patients with severe depression, demonstrated comparable outcomes across both dosage groups, with 67.3% of patients achieving remission by week 8. Adverse events were similar between groups, with minor variations such as increased hyperhidrosis and chest pain in the 120 mg group. Headache and nausea ...

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A search of the published medical literature revealed 2 studies investigating the researchable question:

Are doses greater than 60 mg for Cymbalta (duloxetine) no more effective for MDD or GAD?

Level of evidence
C - Multiple studies with limitations or conflicting results  

READ MORE→

[1] Kornstein SG, Dunner DL, Meyers AL, et al. A randomized, double-blind study of increasing or maintaining duloxetine dose in patients without remission of major depressive disorder after initial duloxetine therapy. J Clin Psychiatry. 2008;69(9):1383-1392. doi:10.4088/jcp.v69n0905
[2] Brecht S, Desaiah D, Marechal ES, Santini AM, Podhorna J, Guelfi JD. Efficacy and safety of duloxetine 60 mg and 120 mg daily in patients hospitalized for severe depression: a double-blind randomized trial. J Clin Psychiatry. 2011;72(8):1086-1094. doi:10.4088/JCP.09m05723blu
[3] Alaka KJ, Noble W, Montejo ...

InpharmD's Answer GPT's Answer

Author:Muna Said, PharmD, BCPS + InpharmD™ AI

INTRODUCTION BY INPHARMD™ RESEARCHER

Limited data from observational studies (Tables 1-4) demonstrate prophylactic use of enoxaparin in hemodialysis patients to have similar efficacy compared to UFH, along with comparable bleeding and thrombotic outcomes. While an ideal dosing regimen for DVT prophylaxis in patients on hemodialysis has not yet been established, individualized strategies and careful monitoring are recommended while administering enoxaparin in this patient population.

A 2022 systematic review and network meta-analysis assessed the efficacy and safety of anticoagulants for the treatment and prophylaxis of venous thromboembolism (VTE) in patients with renal dysfunction. This comprehensive analysis included 21 randomized controlled trials with a total of 76,574 participants, among whom 8,972 exhibited renal insufficiency, including VTE prophylaxis (N= 7 trials). In the prophylaxis of VTE, desirudin demonstrated a lower risk of VTE occurrence compared to enoxaparin, though it was associated with a higher bleeding risk. Conversely, betrixaban emerged as the most favorable anticoagulant for prophylaxis due to its superior safety and efficacy profile. Among the various anticoagulants studied, enoxaparin was specifically compared concerning its use in patients undergoing hemodialysis. Enoxaparin, when used in such patients, requires careful consideration due to potential challenges in balancing efficacy and the risk of bleeding. The analysis emphasized t...

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A search of the published medical literature revealed 4 studies investigating the researchable question:

Can enoxaparin be used for DVT prophylaxis in a patient on hemodialysis?

Level of evidence
C - Multiple studies with limitations or conflicting results  

READ MORE→

[1] Fan G, Wang D, Zhang M, Luo X, Zhai Z, Wu S. Anticoagulant for treatment and prophylaxis of venous thromboembolism patients with renal dysfunction: A systematic review and network meta-analysis. Front Med (Lausanne). 2022;9:979911. Published 2022 Sep 26. doi:10.3389/fmed.2022.979911
[2] Shaikh SA, Regal RE. Dosing of Enoxaparin in Renal Impairment. P T. 2017;42(4):245-249.
[3] Lai S, Coppola B. Use of enoxaparin in end-stage renal disease. Kidney Int. 2013;84(3):433-436. doi:10.1038/ki.2013.163
[4] Davenport A. What are the anticoagulation options for intermittent hemodialysis?. Nat ...

Find answers, not documents.

Before InpharmD™


BeforeTime
Your team spends hours per week cobbling together literature from different studies, many behind paywalls, leaving little time for action.
BeforeTime
TI opportunities are discovered (or presented by third parties) months after the fact, resulting in costly missed savings.
BeforeTime
Decisions may be made without a complete picture, or pushed out while gathering consensus.

After InpharmD™


BeforeTime
InpharmD™ delivers customized, actionable drug information in real time, so you can focus on execution.
BeforeTime
Your team stays informed immediately when new data emerges or prices change, and you’ll always be the first to know when any changes impact your formulary.
BeforeTime
With InpharmD™, your team can make faster, more informed decisions and move forward with confidence.

What Clinical Pharmacists Are Saying...


     

Assists in our research and is a great way or us to get an answer to a medical question without spending an average of 2 hours researching UptoDate or PubMed ourselves.


  Jordan C., PharmD, New Jersey

     

Huge time saver with thorough responses.


  Jane D., PharmD, Georgia

     

I’d never heard of a DI pharmacist before, now I have one. In. My. Pocket. Amazing!


     

Holy Shhh. Cow! Holy Cow! These summaries are beautiful.


  Jane D., PharmD, Georgia

     

I just want to say: This is such a brilliant idea! You people are genius.


     

OH MY GOD WHERE HAVE YOU BEEN ALL MY LIFE!


     

I can’t tell you how much time I spend literature searching. And how I CANNOT STAND PAYWALLS. THIS IS UNBELIEVABLE!! (covers face for sec) thank you, thank you, thank you!


     

So they’re basically connecting academic researchers with front line providers and then automating everything. It’s simply brilliant.


     

The clinical pharmacist was our secret weapon anyway. (Smiles wryly) This pharmacist AI seems superhuman. I’m just blown away, honestly. (Looks at camera somberly.)


     

It’s an ENTIRE DI DEPARTMENT, that lives in Epic. Give me a second. I’m just having a hard time wrapping my head around that.


     

Sorry just give me a second, my mind is blown.


     

Stop reading and just download the app already! I’ve tried all of them. This is by far the most advanced, best-in-class.


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