Diphenhydramine API from Indian Manufacturers & Suppliers

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Commercial-scale Suppliers

Pharm Rx Chemical Corp

Distributor

Produced in China

Employees: 50+

Audit Report:

Certifications: GMP

USDMF

MSDS

BSE/TSE

CoA

All certificates

GMP

USDMF

MSDS

BSE/TSE

CoA

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Chr. Olesen Group

Distributor

Produced in India

Employees: 150

Audit Report:

Certifications: GMP

CEP

MSDS

CoA

All certificates

GMP

CEP

MSDS

CoA

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Apollo Healthcare Resources (Singapore)

Distributor

Produced in Singapore

Employees: 50+

Audit Report:

Certifications: GMP

FDA

CEP

USDMF

EDMF/ASMF

All certificates

GMP

FDA

CEP

USDMF

EDMF/ASMF

MSDS

BSE/TSE

ISO9001

JDMF

KDMF

CoA

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Aurora Industry Co., Ltd

Distributor

Produced in China

Employees: 50+

Audit Report:

Certifications: GMP

CEP

MSDS

BSE/TSE

ISO9001

All certificates

GMP

CEP

MSDS

BSE/TSE

ISO9001

CoA

HALAL

Kosher

ISO14001

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AXXO GmbH

Distributor

Produced in World

Employees: 50

Audit Report:

Certifications: GMP

CEP

USDMF

MSDS

CoA

All certificates

GMP

CEP

USDMF

MSDS

CoA

ISO9001

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Rochem International, Inc.

Distributor

Produced in United States

Employees: 50+

Audit Report:

Certifications: GMP

MSDS

BSE/TSE

ISO9001

CoA

All certificates

GMP

MSDS

BSE/TSE

ISO9001

CoA

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€399,-

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LGM Pharma

Distributor

Produced in World

Employees: 200+

Audit Report:

Certifications: GMP

CEP

USDMF

MSDS

BSE/TSE

All certificates

GMP

CEP

USDMF

MSDS

BSE/TSE

CoA

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Recordati S.p.A.

Producer

Produced in Italy

Audit Report:

Certifications: FDA

CEP

USDMF

coa

All certificates

FDA

CEP

USDMF

coa

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Wanbury

Producer

Produced in India

Audit Report:

Certifications: GMP

FDA

CEP

USDMF

All certificates

GMP

FDA

CEP

USDMF

coa

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Albemarle

Producer

Produced in United States

Audit Report:

Certifications: USDMF

CoA

All certificates

USDMF

CoA

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Medinex Labs.

Producer

Produced in India

Audit Report:

Certifications: GMP

CoA

All certificates

GMP

CoA

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Shanghai Wonder Pharma

Producer

Produced in China

Audit Report:

Certifications: WC

CoA

All certificates

CoA

Request a quote

Kongo Chemical

Producer

Produced in Japan

Audit Report:

Certifications: USDMF

CoA

All certificates

USDMF

CoA

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M2i Life

Producer

Produced in France

Audit Report:

Certifications: coa

All certificates

coa

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Diphenhydramine | CAS No: 58-73-1 | GMP-certified suppliers

A medication that provides symptomatic relief of common allergic conditions, itching, and rashes while also supporting short‑term management of insomnia, motion sickness, and nausea.

Therapeutic categories

Agents producing tachycardiaAminesAminoalkyl EthersAnestheticsAnesthetics, LocalAnti-Allergic Agents

Generic name

Diphenhydramine

Molecule type

small molecule

CAS number

58-73-1

DrugBank ID

DB01075

Approval status

Approved drug, Investigational drug

ATC code

D04AA32

Primary indications

Diphenhydramine is a first-generation histamine H1 receptor antagonist (H1 antihistamine) that is widely available as a non-prescription, over-the-counter (OTC) medication
As an OTC medication, diphenhydramine is typically formulated as tablets and creams indicated for use in treating sneezing, runny nose, itchy/watery eyes, itching of nose or throat, insomnia, pruritis, urticaria, insect bites/stings, allergic rashes, and nausea
Additionally, when the use of oral diphenhydramine is impractical, there are also prescription-only formulations such as diphenhydramine injection products that are effective in adults and pediatric patients (other than premature infants and neonates) for:
I) the amelioration of allergic reactions to blood or plasma, in anaphylaxis as an adjunct to epinephrine and other standard measures after acute allergic reaction symptoms have been controlled, and for other uncomplicated allergic conditions of the immediate type when oral therapy is impossible or contraindicated

Product Snapshot

Diphenhydramine is a small-molecule antihistamine supplied in extensive oral, topical, and parenteral formulations, including OTC solids/liquids and prescription injectable solutions
It is used for allergic symptom management, pruritic conditions, motion sickness, and select situations where parenteral antihistaminic or anticholinergic activity is required
The API supports products authorized in the US and Canada, with both established OTC approvals and certain investigational listings

Clinical Overview

Diphenhydramine (CAS 58-73-1) is a first‑generation antihistamine used for symptomatic relief of allergic conditions including rhinitis, conjunctival irritation, pruritus, urticaria, and reactions to insect bites or stings. It is also used for short‑term management of insomnia, motion sickness, nausea, and cough associated with upper respiratory irritation. Parenteral formulations are employed when oral administration is not feasible, including as adjunctive therapy in acute allergic reactions, for motion sickness, and in selected cases of parkinsonism. It is widely recognized in global markets under long‑standing brands such as Benadryl.

Its pharmacologic activity is driven by inverse agonism at H1 receptors located in respiratory smooth muscle, vascular endothelium, gastrointestinal tissue, cardiac tissue, immune cells, the uterus, and the central nervous system. Blockade of these receptors reduces vascular permeability, vasodilation, and sensory nerve stimulation, thereby moderating histamine‑mediated allergic responses. Central H1 antagonism contributes to its sedative, hypnotic, and antitussive properties.

Diphenhydramine also exerts antimuscarinic effects through competitive antagonism of muscarinic acetylcholine receptors, a feature that supports its use in parkinsonism and contributes to anti‑vertigo and antiemetic actions. Additional activity as a sodium channel blocker has been associated with local anesthetic effects.

Absorption is rapid after oral administration, and its ability to cross the blood–brain barrier leads to pronounced central nervous system effects. Diphenhydramine undergoes hepatic metabolism, including CYP2D6‑mediated pathways, with metabolites excreted primarily in urine. Sedation, cognitive impairment, anticholinergic effects, paradoxical excitation in pediatric patients, and potential QTc prolongation are clinically relevant safety considerations.

For API procurement, suppliers should provide evidence of compliance with pharmacopeial monographs, validated impurity controls consistent with first‑generation antihistamines, and robust management of polymorphism and particle‑size attributes to support consistent formulation performance.

Identification & chemistry

Generic name	Diphenhydramine
Molecule type	Small molecule
CAS	58-73-1
UNII	8GTS82S83M
DrugBank ID	DB01075

Pharmacology

Summary	Diphenhydramine is an inverse agonist of H1 receptors that attenuates histamine‑mediated vascular permeability, smooth muscle activation, and sensory nerve stimulation. It readily enters the CNS, where H1 antagonism produces sedative effects and contributes to antiemetic and antitussive activity. The drug also exhibits antimuscarinic actions and sodium channel blockade, supporting additional effects on vestibular pathways, motor control, and local anesthesia.
Mechanism of action	Diphenhydramine predominantly works via the antagonism of H1 (Histamine 1) receptors . Such H1 receptors are located on respiratory smooth muscles, vascular endothelial cells, the gastrointestinal tract (GIT), cardiac tissue, immune cells, the uterus, and the central nervous system (CNS) neurons . When the H1 receptor is stimulated in these tissues it produces a variety of actions including increased vascular permeability, promotion of vasodilation causing flushing, decreased atrioventricular (AV) node conduction time, stimulation of sensory nerves of airways producing coughing, smooth muscle contraction of bronchi and the GIT, and eosinophilic chemotaxis that promotes the allergic immune response . Ultimately, diphenhydramine functions as an inverse agonist at H1 receptors, and subsequently reverses effects of histamine on capillaries, reducing allergic reaction symptoms . Moreover, since diphenhydramine is a first-generation antihistamine, it readily crosses the blood-brain barrier and inversely agonizes the H1 CNS receptors, resulting in drowsiness, and suppressing the medullary cough center . Furthermore, H1 receptors are similar to muscarinic receptors . Consequently, diphenhydramine also acts as an antimuscarinic . It does so by behaving as a competitive antagonist of muscarinic acetylcholine receptors, resulting in its use as an antiparkinson medication . Lastly, diphenhydramine has also demonstrated activity as an intracellular sodium channel blocker, resulting in possible local anesthetic properties .
Pharmacodynamics	Diphenhydramine has anti-histaminic (H1-receptor), anti-emetic, anti-vertigo and sedative and hypnotic properties . The anti-histamine action occurs by blocking the spasmogenic and congestive effects of histamine by competing with histamine for H1 receptor sites on effector cells, preventing but not reversing responses mediated by histamine alone . Such receptor sites may be found in the gut, uterus, large blood vessels, bronchial muscles, and elsewhere . Anti-emetic action is by inhibition at the medullary chemoreceptor trigger zone . Anti-vertigo action is by a central antimuscarinic effect on the vestibular apparatus and the integrative vomiting center and medullary chemoreceptor trigger zone of the midbrain .

Targets

Target	Organism	Actions
Histamine H1 receptor	Humans	antagonist
Muscarinic acetylcholine receptor M2	Humans	antagonist

ADME / PK

Absorption	Diphenhydramine is quickly absorbed after oral administration with maximum activity occurring in approximately one hour . The oral bioavailability of diphenhydramine has been documented in the range of 40% to 60%, and peak plasma concentration occurs about 2 to 3 hours after administration .
Half-life	The elimination half-life ranges from 2.4-9.3 hours in healthy adults . The terminal elimination half-life is prolonged in liver cirrhosis .
Protein binding	Some prescribing information records the protein binding of diphenhydramine as approximately 78% while others have suggested the medication is about 80 to 85% bound to plasma proteins.
Metabolism	Diphenhydramine undergoes rapid and extensive first-pass metabolism . In particular, two successive N-demethylations occur wherein diphenhydramine is demethylated to N-desmethyldiphenhydramine (the N-desmethyl metabolite) and then this metabolite is itself demethylated to N,N-didesmethyldiphenhydramine (the N,N-didesmethyl metabolite) . Subsequently, acetyl metabolites like N-acetyl-N-desmethyldiphenhydramine are generated via the amine moiety of the N,N-didesmethyl metabolite . Additionally, the N,N-didesmethyl metabolite also undergoes some oxidation to generate the diphenylmethoxyacetic acid metabolite as well . The remaining percentage of a dose of administered diphenhydramine is excreted unchanged . The metabolites are further conjugated with glycine and glutamine and excreted in urine . Moreover, studies have determined that a variety of cytochrome P450 isoenzymes are involved in the N-demethylation that characterizes the primary metabolic pathway of diphenhydramine, including CYP2D6, CYP1A2, CYP2C9, and CYP2C19 . In particular, CYP2D6 demonstrates higher affinity catalysis with the diphenhydramine substrate than the other isoenzymes identified . Consequently, inducers or inhibitors of these such CYP enzymes may potentially affect the serum concentration and incidence and/or severity of adverse effects associated with exposure to diphenhydramine .
Route of elimination	The metabolites of diphenhydramine are conjugated with glycine and glutamine and excreted in urine . Only about 1% of a single dose is excreted unchanged in urine . The medication is ultimately eliminated by the kidneys slowly, mainly as inactive metabolites .
Volume of distribution	Diphenhydramine is widely distributed throughout the body, including the CNS . Following a 50 mg oral dose of diphenhydramine, the volume of distribution is in the range of 3.3 - 6.8 l/kg .
Clearance	Values for plasma clearance of a 50 mg oral dose of diphenhydramine has been documented as lying in the range of 600-1300 ml/min .

Formulation & handling

Oral formulations may require solubilization strategies due to low aqueous solubility and moderate lipophilicity.
Parenteral solutions need appropriate solvents and pH control to maintain solubility and prevent precipitation.
Topical products leverage the lipophilic nature of the API for dermal penetration and generally have fewer stability constraints than aqueous oral liquids.

Regulatory status

Lifecycle	The API’s key U.S. patents expired in 2022, indicating that the product is now in a post‑exclusivity phase. With current marketing limited to the US and Canada, the asset sits in a mature stage of its lifecycle with established generic entry likely.

Markets	US, Canada

Supply Chain

Supply chain summary	Diphenhydramine originated with a single innovator but is now supplied entirely through a broad network of repackagers and generic manufacturers. Branded and private‑label products are widely established in the US and Canada, with no meaningful originator exclusivity remaining. The listed formulation‑related patents expired in 2022, aligning with the mature generic competition already present across the market.

Supply chain summary

Diphenhydramine originated with a single innovator but is now supplied entirely through a broad network of repackagers and generic manufacturers. Branded and private‑label products are widely established in the US and Canada, with no meaningful originator exclusivity remaining. The listed formulation‑related patents expired in 2022, aligning with the mature generic competition already present across the market.

Safety

Toxicity	Overdose is expected to result in effects similar to the adverse effects that are ordinarily associated with the use of diphenhydramine, including drowsiness, hyperpyrexia, and anticholinergic effects, among others . Additional symptoms during overdose may include mydriasis, fever, flushing, agitation, tremor, dystonic reactions, hallucinations and ECG changes . Large overdose may cause rhabdomyolysis, convulsions, delirium, toxic psychosis, arrhythmias, coma and cardiovascular collapse . Moreover, with higher doses, and particularly in children, symptoms of CNS excitation including hallucinations and convulsions may appear; with massive doses, coma or cardiovascular collapse may follow . Although diphenhydramine has been in widespread use for many years without ill consequence, it is known to cross the placenta and has been detected in breast milk . This medication should therefore only be used when the potential benefit of treatment to the mother exceeds any possible hazards to the developing fetus or suckling infant . Pharmacokinetic studies indicate no major differences in the distribution or elimination of diphenhydramine compared to younger adults . Nevertheless, diphenhydramine should be used with caution in the elderly, who are more likely to experience adverse effects . Avoid use in elderly patients with confusion . The results of a review on the use of diphenhydramine in renal failure suggest that in moderate to severe renal failure, the dose interval should be extended by a period dependent on Glomerular filtration rate (GFR) . After intravenous administration of 0.8 mg/kg diphenhydramine, a prolonged half-life was noted in patients with chronic liver disease which correlated with the severity of the disease . However, the mean plasma clearance and apparent volume of distribution were not significantly affected . LD<sub>50</sub>=500 mg/kg (orally in rats). Considerable overdosage can lead to myocardial infarction (heart attack), serious ventricular dysrhythmias, coma and death.

Toxicity

Overdose is expected to result in effects similar to the adverse effects that are ordinarily associated with the use of diphenhydramine, including drowsiness, hyperpyrexia, and anticholinergic effects, among others . Additional symptoms during overdose may include mydriasis, fever, flushing, agitation, tremor, dystonic reactions, hallucinations and ECG changes . Large overdose may cause rhabdomyolysis, convulsions, delirium, toxic psychosis, arrhythmias, coma and cardiovascular collapse . Moreover, with higher doses, and particularly in children, symptoms of CNS excitation including hallucinations and convulsions may appear; with massive doses, coma or cardiovascular collapse may follow . Although diphenhydramine has been in widespread use for many years without ill consequence, it is known to cross the placenta and has been detected in breast milk . This medication should therefore only be used when the potential benefit of treatment to the mother exceeds any possible hazards to the developing fetus or suckling infant . Pharmacokinetic studies indicate no major differences in the distribution or elimination of diphenhydramine compared to younger adults . Nevertheless, diphenhydramine should be used with caution in the elderly, who are more likely to experience adverse effects . Avoid use in elderly patients with confusion . The results of a review on the use of diphenhydramine in renal failure suggest that in moderate to severe renal failure, the dose interval should be extended by a period dependent on Glomerular filtration rate (GFR) . After intravenous administration of 0.8 mg/kg diphenhydramine, a prolonged half-life was noted in patients with chronic liver disease which correlated with the severity of the disease . However, the mean plasma clearance and apparent volume of distribution were not significantly affected . LD<sub>50</sub>=500 mg/kg (orally in rats). Considerable overdosage can lead to myocardial infarction (heart attack), serious ventricular dysrhythmias, coma and death.

High Level Warnings:

Significant overdose may elicit pronounced anticholinergic and CNS toxicity, including agitation, hallucinations, tremor, dystonic reactions, ECG abnormalities, arrhythmias, and risk of coma or cardiovascular collapse
Prolonged half‑life is reported in chronic liver disease
Altered clearance profiles may also occur in moderate to severe renal impairment

Diphenhydramine is a type of Antihistamines

Antihistamines are a vital subcategory of pharmaceutical Active Pharmaceutical Ingredients (APIs) widely used in the treatment of allergies and allergic reactions. These compounds work by blocking the action of histamines, which are responsible for triggering allergic symptoms such as itching, sneezing, runny nose, and watery eyes.

Antihistamines can be classified into two main categories: first-generation and second-generation antihistamines. First-generation antihistamines, such as diphenhydramine and chlorpheniramine, have been in use for several decades. They are effective in relieving allergy symptoms but are associated with drowsiness and other side effects due to their ability to cross the blood-brain barrier.

On the other hand, second-generation antihistamines, including cetirizine, loratadine, and fexofenadine, offer similar allergy relief with fewer sedative effects. These newer antihistamines are preferred for their improved safety profiles, making them suitable for use during the day without causing significant drowsiness.

Antihistamines are available in various forms, including tablets, capsules, syrups, and topical creams. They are extensively used to manage conditions such as hay fever, hives, allergic rhinitis, and insect bites. Moreover, antihistamines may also be combined with decongestants or other medications to provide relief from nasal congestion and sinus symptoms.

As pharmaceutical APIs, antihistamines are produced through meticulous synthesis and manufacturing processes, adhering to strict quality standards. These APIs serve as the active components in various branded and generic pharmaceutical formulations, making them crucial in the pharmaceutical industry's production of allergy medications.

In conclusion, antihistamines are a significant subcategory of pharmaceutical APIs widely used for alleviating allergy symptoms. Their classification into first- and second-generation antihistamines offers options based on efficacy and sedative effects. By blocking histamines, antihistamines provide relief from common allergic reactions, making them essential in the development of effective allergy medications.

Diphenhydramine (Antihistamines), classified under Central Nervous System Agents

Central Nervous System (CNS) Agents are a crucial category of pharmaceutical Active Pharmaceutical Ingredients (APIs) that specifically target the central nervous system. The CNS encompasses the brain and spinal cord, playing a vital role in regulating and controlling various bodily functions, including cognition, movement, emotions, and sensory perception. These agents are designed to interact with specific receptors, enzymes, or ion channels within the CNS to modulate neural activity and restore normal functioning.

CNS agents comprise a diverse range of pharmaceutical APIs, including analgesics, anesthetics, antipsychotics, sedatives, hypnotics, anti-epileptics, and antidepressants. Each subcategory addresses distinct neurological disorders and conditions. For instance, analgesics alleviate pain by targeting receptors in the brain and spinal cord, while antipsychotics are employed to manage psychosis symptoms in mental illnesses such as schizophrenia.

The development of CNS agents involves rigorous research, molecular modeling, and extensive clinical trials to ensure safety, efficacy, and specific target engagement. Pharmaceutical companies invest significant resources in identifying novel drug targets, synthesizing new compounds, and optimizing their pharmacological properties. These agents undergo rigorous regulatory evaluations and must adhere to stringent quality standards and guidelines.

Given the prevalence of CNS disorders globally, the market demand for effective CNS agents is substantial. The development of innovative CNS APIs not only improves patient outcomes but also provides valuable commercial opportunities for pharmaceutical companies. Continued advancements in CNS agent research and development hold the promise of groundbreaking therapies that can improve the quality of life for individuals affected by neurological conditions.

Diphenhydramine API manufacturers & distributors

Compare qualified Diphenhydramine API suppliers worldwide. We currently have 14 companies offering Diphenhydramine API, with manufacturing taking place in 8 different countries. Use the table below to review supplier type, countries of origin, certifications, product portfolio and GMP audit availability.

Supplier	Type	Country	Product origin	Certifications	Portfolio
Albemarle	Producer	United States	United States	CoA, USDMF	17 products
Apollo Healthcare Resourc...	Distributor	Singapore	Singapore	BSE/TSE, CEP, CoA, EDMF/ASMF, FDA, GMP, ISO9001, JDMF, KDMF, MSDS, USDMF, WC	200 products
Aurora Industry Co., Ltd	Distributor	China	China	BSE/TSE, CEP, CoA, GMP, HALAL, ISO14001, ISO9001, Kosher, MSDS	250 products
AXXO GmbH	Distributor	Germany	World	CEP, CoA, GMP, GDP, MSDS, USDMF	243 products
Chr. Olesen Group	Distributor	Denmark	India	CEP, CoA, GMP, MSDS	252 products
Kongo Chemical	Producer	Japan	Japan	CoA, USDMF	5 products
LGM Pharma	Distributor	United States	World	BSE/TSE, CEP, CoA, GMP, MSDS, USDMF	441 products
M2i Life	Producer	France	France	CoA	1 products
Medinex Labs.	Producer	India	India	CoA, GMP, WC	8 products
Pharm Rx Chemical Corp	Distributor	United States	China	BSE/TSE, CoA, GMP, MSDS, USDMF	166 products
Recordati S.p.A.	Producer	Italy	Italy	CEP, CoA, FDA, USDMF	18 products
Rochem International, Inc...	Distributor	United States	United States	BSE/TSE, CoA, GMP, ISO9001, MSDS	144 products
Shanghai Wonder Pharma	Producer	China	China	CoA, WC	5 products
Wanbury	Producer	India	India	CEP, CoA, FDA, GMP, USDMF, WC	15 products

When sending a request, specify which Diphenhydramine API quality you need: for example EP (Ph. Eur.), USP, JP, BP, or another pharmacopoeial standard, as well as the required grade (base, salt, micronised, specific purity, etc.).

Use the list above to find high-quality Diphenhydramine API suppliers. For example, you can select GMP, FDA or ISO certified suppliers. Visit our help page to learn more about sourcing APIs via Pharmaoffer.

Frequently asked questions about Diphenhydramine API

Sourcing

What matters most when sourcing GMP-grade Diphenhydramine?

The key considerations are confirmed GMP compliance and alignment with US and Canadian regulatory expectations. A stable, traceable supply chain is important because material now comes from multiple repackagers and generic manufacturers. With patent protections expired and broad generic availability, consistency of quality documentation and reliable batch-to-batch performance are central to sourcing decisions.

Which documents are typically required when sourcing Diphenhydramine API?

Request the core API documentation set: CoA (14 companies), GMP (9 companies), USDMF (8 companies), CEP (7 companies), MSDS (7 companies). Confirm versions and validity dates match the destination market to avoid delays in qualification.

Which manufacturers are known to produce Diphenhydramine API?

Known or reported manufacturers for Diphenhydramine: Chr. Olesen Group, Aurora Industry Co., Ltd, Pharm Rx Chemical Corp, Apollo Healthcare Resources (Singapore), LGM Pharma, AXXO GmbH, Rochem International, Inc.. Evaluate their GMP history, scale, and regional coverage before requesting dossiers or allocating demand.

How can I request quotes for Diphenhydramine API from GMP suppliers?

Submit quote requests through the supplier listings with your specs and required documents (specifications, target volume, delivery timeline, and destination). Providing consistent details upfront speeds comparable offers and clarifies technical feasibility.

Is a GMP audit report available for Diphenhydramine manufacturers?

Audit reports may be requested for Diphenhydramine: 4 GMP audit reports available. Confirm the scope and recency of any audit before relying on it for qualification decisions.

How many suppliers offer Diphenhydramine API on Pharmaoffer?

Reported supplier count for Diphenhydramine: 14 verified suppliers. Filter listings by certifications, regions, and delivery options to match your qualification plan.

Which countries are known to manufacture Diphenhydramine API?

Production countries reported for Diphenhydramine: India (3 producers), China (3 producers), United States (2 producers). Knowing the manufacturing geography helps anticipate logistics lead times and import compliance needs.

Which certifications do suppliers of Diphenhydramine usually hold?

Common certifications for Diphenhydramine suppliers: CoA (14 companies), GMP (9 companies), USDMF (8 companies), CEP (7 companies), MSDS (7 companies). Always verify issuing authorities and expiry dates when reviewing audit packages.

Technical

What is Diphenhydramine (CAS 58-73-1) used for?

Diphenhydramine is used for symptomatic relief of allergic conditions such as rhinitis, conjunctival irritation, pruritus, urticaria, and reactions to insect bites or stings. It is also used for short‑term management of insomnia, motion sickness, nausea, and cough associated with upper respiratory irritation. Parenteral forms serve as adjunct therapy in acute allergic reactions and are used when oral dosing is not feasible, including for motion sickness and selected cases of parkinsonism.

Which therapeutic class does Diphenhydramine fall into?

Diphenhydramine belongs to the following therapeutic categories: Agents producing tachycardia, Amines, Aminoalkyl Ethers, Anesthetics, Anesthetics, Local. This positioning helps teams compare alternative APIs, anticipate pharmacology expectations, and align early research priorities.

What conditions is Diphenhydramine mainly prescribed for?

The primary indications for Diphenhydramine: Diphenhydramine is a first-generation histamine H1 receptor antagonist (H1 antihistamine) that is widely available as a non-prescription, over-the-counter (OTC) medication, As an OTC medication, Diphenhydramine is typically formulated as tablets and creams indicated for use in treating sneezing, runny nose, itchy/watery eyes, itching of nose or throat, insomnia, pruritis, urticaria, insect bites/stings, allergic rashes, and nausea, Additionally, when the use of oral Diphenhydramine is impractical, there are also prescription-only formulations such as Diphenhydramine injection products that are effective in adults and pediatric patients (other than premature infants and neonates) for:, I) the amelioration of allergic reactions to blood or plasma, in anaphylaxis as an adjunct to epinephrine and other standard measures after acute allergic reaction symptoms have been controlled, and for other uncomplicated allergic conditions of the immediate type when oral therapy is impossible or contraindicated. These use cases frame the target patient populations and help prioritize formulation and safety evaluations.

How does Diphenhydramine work?

Diphenhydramine predominantly works via the antagonism of H1 (Histamine 1) receptors . Such H1 receptors are located on respiratory smooth muscles, vascular endothelial cells, the gastrointestinal tract (GIT), cardiac tissue, immune cells, the uterus, and the central nervous system (CNS) neurons . When the H1 receptor is stimulated in these tissues it produces a variety of actions including increased vascular permeability, promotion of vasodilation causing flushing, decreased atrioventricular (AV) node conduction time, stimulation of sensory nerves of airways producing coughing, smooth muscle contraction of bronchi and the GIT, and eosinophilic chemotaxis that promotes the allergic immune response . Ultimately, Diphenhydramine functions as an inverse agonist at H1 receptors, and subsequently reverses effects of histamine on capillaries, reducing allergic reaction symptoms . Moreover, since Diphenhydramine is a first-generation antihistamine, it readily crosses the blood-brain barrier and inversely agonizes the H1 CNS receptors, resulting in drowsiness, and suppressing the medullary cough center . Furthermore, H1 receptors are similar to muscarinic receptors . Consequently, Diphenhydramine also acts as an antimuscarinic . It does so by behaving as a competitive antagonist of muscarinic acetylcholine receptors, resulting in its use as an antiparkinson medication . Lastly, Diphenhydramine has also demonstrated activity as an intracellular sodium channel blocker, resulting in possible local anesthetic properties .

What should someone know about the safety or toxicity profile of Diphenhydramine?

Diphenhydramine commonly causes sedation, cognitive slowing, and anticholinergic effects such as dry mouth, blurred vision, constipation, and urinary retention. Significant overdose can lead to severe anticholinergic and central nervous system toxicity, including agitation, hallucinations, tremor, dystonic reactions, ECG abnormalities, arrhythmias, coma, or cardiovascular collapse. QTc prolongation and paradoxical excitation in pediatric patients are noted risks. Reduced clearance may occur in chronic liver disease or moderate to severe renal impairment, increasing exposure.

What are important formulation and handling considerations for Diphenhydramine as an API?

Formulation of Diphenhydramine typically addresses its low aqueous solubility by using solubilizers or suitable vehicles for oral products, and pH control with appropriate solvents for parenteral solutions to avoid precipitation. Its moderate lipophilicity supports topical formulations that rely on dermal penetration and have fewer stability challenges than aqueous oral liquids. Handling should maintain conditions that preserve solubility and prevent physical instability in the chosen dosage form.

Is Diphenhydramine a small molecule?

Diphenhydramine is classified as a small molecule. That classification shapes process design, impurity profiling, and analytical control strategies.

Are there special stability concerns for oral Diphenhydramine?

Oral Diphenhydramine has low aqueous solubility, so formulations may require solubilization strategies to maintain uniformity and prevent precipitation. Aqueous oral liquids can be more prone to stability issues than topical products because of this solubility limitation. pH control and appropriate excipients help maintain the API in solution throughout shelf life. No additional stability concerns are noted beyond managing its limited solubility.

Regulatory

Where is Diphenhydramine approved or in use globally?

Diphenhydramine is reported as approved in the following major regions: US, Canada. Understanding geographic coverage informs regulatory filings, supply planning, and risk assessments before escalating procurement.

What’s the regulatory and patent landscape for Diphenhydramine right now?

In the US and Canada, Diphenhydramine is regulated as an established active ingredient within standard national frameworks. The context indicates no special regulatory restrictions beyond routine oversight. The provided information does not reference any active patents, implying no patent‑related limitations within this context.

Pharmaoffer

How does Pharmaoffer’s Smart Sourcing Service help with Diphenhydramine procurement?

Pharmaoffer's Smart Sourcing Service coordinates compliant suppliers, documentation, and competitive quotes for Diphenhydramine. It centralizes outreach, follow-ups, and document validation to shorten procurement timelines.

Is Diphenhydramine included in the PRO Data Insights coverage?

PRO Data Insights coverage for Diphenhydramine: 3569 verified transactions across 808 suppliers and 425 buyers worldwide. Use the dataset to benchmark suppliers and monitor regulatory activity where available.

Where can I access the API market report for Diphenhydramine?

Market report availability for Diphenhydramine: . The report highlights demand trends, pricing drivers, and supplier landscape insights for procurement planning.