Metal complexes of carboxamidrazone analogs as antitubercular agents: 1. Synthesis, X-ray crystal-structures, spectroscopic properties and antimycobacterial activity against Mycobacterium tuberculosis H37Rv

N¹-Benzylidene-pyridine carboxamidrazones and their metal conjugates have emerged as a new class of potential antimycobacterial agents. Nine such carboxamidrazone analogs (L₁–L₉) along with their Cu(II) (MC₁–MC₉) and Fe(III) (MC₁₀–MC₁₈) complexes were synthesized. Single crystal X-ray structures of copper complexes MC₁ and MC₅ were determined which suggest slightly distorted square planer geometries for copper complexes and octahedral geometries for ferric compounds. All compounds were evaluated for their in vitro antimycobacterial activity against Mycobacterium tuberculosis H₃₇Rv. The results show 32–64-fold enhancement in antitubercular activity upon copper complexation.     

Synthesis, spectral studies and in vitro assessment for antiamoebic activity of new cyclooctadiene ruthenium(II) complexes with 5-nitrothiophene-2-carboxaldehyde thiosemicarbazones

We report here the synthesis, characterization and in vitro antiamoebic activity of 5-nitrothiophene-2-carboxaldehyde thiosemicarbazones (TSC), 1–5, and their bidentate complexes [Ru(η⁴-C₈H₁₂)(TSC)Cl₂] 1a–5a. The biological studies of these compounds were investigated against HK-9 strain of Entamoeba histolytica and the concentration causing 50% cell growth inhibition (IC₅₀) was calculated in the micromolar range. The ligands exhibited antiamoebic activity in the range (2.05–5.29 μM). Screening results indicated that the potencies of the compounds increased by the incorporation of ruthenium(II) in the thiosemicarbazones. The complexes 1a–5a showed antiamoebic activity with an IC₅₀ of 0.61–1.43 μM and were better inhibitors of growth of E. histolytica, based on IC₅₀ values. The most promising among them is Ru(II) complex 2a having 1,2,3,4-tetrahydroquinoline as N⁴ substitution.     

Synthesis, characterization and reactivity of platinum-substituted ketenes [PtX{η-C(PPh3)CO}L2]BF4, (X=Me, Cl; L2=1,5-cyclooctadiene, 1,2-bis(diphenylphosphino)ethane, cis-1,2-bis(diphenylphosphino)ethene). Steric and electronic effects of the ancillary ligands

Ketenylidenetriphenylphosphorane, Ph₃PC=C=O, 1, has been used to synthesize platinum-substituted ketenes [PtMe{η¹-C(PPh₃)CO}L₂]BF₄, 2a, b (L₂=1,5-cyclooctadiene, cod (a), 1,2-bis(diphenylphosphino)ethane, diphos (b)). Parent compound [PtCl{η¹-C(PPh₃)CO}L₂]BF₄, 3, with L₂=cis-1,2-bis(diphenylphosphino)ethene, diphoe, was also synthesized, which is stable only at low temperature. The stability of 2 and 3 and the reactivity of the C=C=O moiety have been examined and discussed in terms of the electronic and steric characteristics of the ancillary ligands, also taking into account the reactivity of the ‘PtXL₂’ fragment with other carbonyl stabilized phosphorus ylides, Ph₃PCHCOR (R=Me, Ph, OMe, OEt).     

Electrospray mass spectrometric investigation of the relative ligand properties of EPh3 ligands (E=P, As, Sb or Bi) towards Ag and Cu

Electrospray mass spectrometry (ESMS) has been used to investigate the relative ligand properties of the triphenylpnictogen ligands EPh₃ (E=P, As, Sb and Bi) towards silver(I) and copper(I) ions. It is found that the preferred species formed increase in coordination number from two for PPh₃ in [Ag(PPh₃)₂]⁺ to four for SbPh₃ in [Ag(SbPh₃)₄]⁺, consistent with the decreasing donor ligand ability and increasing metal –E bond length in the series PPh₃–AsPh₃–SbPh₃. With BiPh_3, the spectra were complex, suggesting considerable decomposition. These studies also suggest that silver(I) and copper(I) ions will have widespread utility in the characterisation of tertiary stibine ligands, as has been described previously for phosphines and arsines. These studies demonstrate the power of the ESMS technique in determining the donor properties of a related series of ligands, and this information is of significance in coordination chemistry.     

Reactivity study of cyclopentadienyl osmium(II) bisphosphine azido complexes with activated alkynes and nitriles: Isolation of osmium triazolato and tetrazolato complexes by 1,3-dipolar addition

The cyclopentadienyl osmium(II) complexes [(η⁵-C₅H₅)Os(PPh₃)₂X] [X = Br (1), CH₃CN (2)] reacts with sodium azide (NaN₃) to yield the corresponding azido complex [(η⁵-C₅H₅)Os(PPh₃)₂N₃] (3). This undergoes [3+2] dipolar cycloaddition reaction with activated alkynes like dimethyl and diethyl acetylenedicarboxylate to yield triazolato complexes [(η⁵-C₅H₅)Os(PPh₃)₂{N₃C₂(CO₂R)₂}] [R = –CH₂CH₃ (4) and –CH₃ (5)]. The complex 3 also reacts with nitriles such as tetracyanoethylene (TCE), fumaronitrile and p-nitrobenzonitrile to yield complexes of the type [(η⁵-C₅H₅)Os(PPh₃)₂{N₄C₂(CN)C(CN)₂}] (6), [(η⁵-C₅H₅)Os(PPh₃)₂{N₃C₂HCN}] (7) and [(η⁵-C₅H₅)Os(PPh₃)₂{N₄C(C₆H₄–p-NO₂)}] (8). These complexes were fully characterized on the basis of microanalyses, FT-IR and NMR spectroscopic data. The molecular structure of the representative complex [(η⁵-C₅H₅)Os(PPh₃)₂{N₃C₂(CO₂CH₂CH₃)₂}] (4) was determined by single crystal X-ray analysis.     

Hydrolysis of fibrinogen and plasminogen by immobilized earthworm fibrinolytic enzyme II from Eisenia fetida

Earthworm fibrinolytic enzyme II (EFE-II) from Eisenia fetida has a broad hydrolytic specificity for peptide bonds. Our experiments show that EFE-II can hydrolyze the specific chromogenic substrates of thrombin (Chromozym TH), trypsin (Chromozym TRY) and elastase (Chromozym ELA). The Michaelis–Menten constant (K_m) for Chromozym ELA (245 μM) is much higher than those for the thrombin (90 μM) and trypsin (60 μM) substrates. On the other hand, EFE-II is inhibited most strongly by soybean trypsin inhibitor (SBTI), and weakly inhibited by elastinal, suggesting that EFE-II has a trypsin-like activity. Degradation of plasminogen (PLg) and fibrinogen by EFE-II was investigated after EFE-II had been immobilized onto 1,1′-carboryl-diimidazole (CDI)-activated Sepharose CL-6B. The immobilized EFE-II has 55–60% activity of the native enzyme with a higher thermal and pH resistance. EFE-II cleaves PLg at four hydrolytic sites: Lys₇₇–Arg₇₈, Arg₃₄₂–Met₃₄₃, Ala₄₄₄–Ala₄₄₅ and Arg₅₅₇–Ile₅₅₈. The site Arg₅₅₇–Ile₅₅₈ is also recognized and cleaved by tissue plasminogen activator (t-PA) and urokinase (UK), producing active plasmin. Cleaving Ala₄₄₄–Ala₄₄₅ released mini-plasmin with secondary activity to hydrolyze fibrin. Immobilized EFE-II degrades not only the A chain of fibrinogen in the C-terminal region (like human neutrophil elastase, HNE), but also in the N-terminal region at the Val₂₁–Glu₂₂ site.     

Surprisingly high stability of barley lipid transfer protein, LTP1, towards denaturant, heat and proteases

Tripeptidyl peptidase-I (TPP-I) is a lysosomal peptidase which cleaves tripeptides from the N-terminus of peptides. The function of the enzyme is unclear but its importance is demonstrated by the fact that mutations in TPP-I are responsible for late infantile neuronal ceroid lipofuscinosis, a lethal lysosomal storage disease. As a step towards identifying its natural substrates, we have used a series of synthetic peptides, based on angiotensin-II, to explore the effects of peptide chain length and the effects of amino acid substitutions at the P₁ and P₁′ positions on the rate of catalysis. With the exception of angiotensin-(1–8) (angiotensin-II), which is a relatively poor substrate for TPP-I, the rate of catalysis increases with increasing chain length. K_cat/K_m values increase 50-fold between angiotensin-(1–5) and angiotensin-(1–14). TPP-I shows little specificity for the nature of the amino acids in the P₁ and P₁′ positions, K_cat/K_m values varying only 5-fold for a range of substitutions. However, Pro or Lys in the P₁ position and Pro in the P₁′ positions are incompatible with TPP-I activity. These observations suggest that TPP-I is a non-specific, but essential, peptidase involved in the latter stages of lysosomal protein degradation.     

不同灌溉畦长对小麦光合特性、干物质积累及水分利用效率的影响

以高产冬小麦品种济麦22为材料,研究不同灌溉畦长对小麦旗叶水势、光合特性和干物质积累与分配的影响.2010—2011年小麦生长季设置畦长为10(L₁₀)、20(L₂₀)、40(L₄₀)、60(L₆₀)、80(L₈₀)和100 m(L₁₀₀)的6个处理,2011—2012年和2012—2013年设置畦长为40(L₄₀)、60(L₆₀)、80(L₈₀)和100 m(L₁₀₀)的4个处理.结果表明: 2010—2011年生长季开花期0～200 cm土层平均土壤相对含水量为L₈₀、L₆₀>L₁₀₀>L₄₀>L₂₀>L₁₀,2011—2012年和2012—2013年为L₈₀、L₆₀>L₁₀₀>L₄₀.开花后11 d和21 d,旗叶水势、净光合速率和蒸腾速率均为L₈₀、L₁₀₀>L₆₀>L₄₀>L₂₀、L₁₀;花后31 d为L₈₀>L₆₀、L₁₀₀>L₄₀、L₂₀、L₁₀.L₈₀各区间开花期和成熟期干物质积累量及籽粒产量变异系数小于L₁₀₀,平均干物质积累量及开花后干物质积累量和对籽粒产量的贡献率显著高于L₁₀₀、L₄₀、L₂₀和L₁₀,平均籽粒产量和水分利用效率显著高于其他处理,是本试验条件下节水高产的最优畦长处理.     

KMI-008, a novel beta-secretase inhibitor containing a hydroxymethylcarbonyl isostere as a transition-state mimic: design and synthesis of substrate-based octapeptides

A novel class of substrate-based β-secretase (BACE1) inhibitors containing a hydroxymethylcarbonyl (HMC) isostere was designed and synthesized. Phenylnorstatine [(2R,3S)-3-amino-2-hydroxy-4-phenylbutyric acid; Pns] was an effective transition-state mimic at the P₁ position. Structure–activity relationships (SARs) of the P₃–P₃′ positions of BACE1 inhibitors were studied.     

Chemistry of vinylidene complexes XI. Synthesis of trinuclear MnFePt complexes by means of consecutive assembling out of mono- and dimetal vinylidene precursors

The dimetal μ-vinylidene complexes Cp(CO)₂MnPt(μ-C = CHPh)L₂ (L = tert.-phosphine or -phosphite), which have been obtained by coupling of the mononuclear complex Cp(CO)₂Mn=C=CHPh and unsaturated PtL₂ unit, add smoothly the Fe(CO)₄ moiety to produce trimetal MnFePt compounds. The μ₃-vinylidene cluster CpMnFePt(μ₃-C=CHPh)(CO)₆(PPh₃) was prepared in quantitative yields from the reactions of Cp(CO)₂MnPt(μ-C=CHPh)(PPh₃)L (L = PPh₃ or CO) with Fe₂(CO)₉ in benzene at 20 °C. The phosphite-substituted complexes Cp(CO)₂Mnpt(μ-C=CHPh)L₂ (L = P(OEt)₃ or P(OPrⁱ)₃) react under analogous conditions with Fe₂(CO)₉ to give mixtures (2:3) of the penta- and hexacarbonyl clusters, CpMnFePt(μ₃-C = CHPh)(CO)₅L₂ and CpMnFePt(μ₃-C = CHPh)(CO)₆L, respectively. The similar reaction of the dimetal complex Cp(CO)₂MnPt(μ-C = CHPh)(dppm), in which the Pt atom is chelated by dppm = Ph₂PCH₂PPhPin2 ligand, gives only a 15% yield of the analogous trimetal μ₃-vinylidene hexacarbonyl product CpMnFePt(μ₃-C = CHPh)(CO)(dppm), but the major product (40%) is the tetranuclear μ₄-vinylidene cluster (dppm)PtFe₃(μ₄-C = CHPh)(CO)₉. The IR and ¹H, ¹³C and ³¹P NMR data for the new complexes are reported and discussed.     

Methylene bridged binuclear bis(imino)pyridyl iron(II) complexes and their use as catalysts together with Al(i-Bu)3 for ethylene polymerization

Three novel methylene bridged binuclear iron(II) complexes: (R,R′ = i-C₃H₇ (6); R = i-C₃H₇, R′ = CH₃ (7); R,R′ = CH₃ (8))} have been synthesized. Activated by Al(i-Bu)₃, complex 6 shows very poor activity for the polymerization of ethylene at one bar ethylene pressure, whereas, 7 and 8 exhibit much higher activity than mononuclear iron catalysts {[ArNC(Me)C₅H₃N(Me)CNAr′]FeCl₂ (Ar,Ar′ = 2,6-C₆H₃-i-Pr (9); Ar = 2,6-C₆H₃-i-Pr₂, Ar′ = 2,6-C₆H₃–Me₂ (10); Ar,Ar′ = 2,6-C₆H₃–Me₂ (11))}. The molecular weight (M_w) of PE produced by 7 and 8 are in the range 13.2–46.0 × 10⁴ and much higher than those produced by mononuclear iron catalysts 9 and 10. GPC results demonstrate that 7 and 8 yield PE with a broad/bimodal molecular weight distribution (MWD). In contrast, 9 and 10 yield PE with relatively narrow and unimodal MWD (4.26 and 3.55). Elevating the temperature and Al/Fe molar ratio will narrow the MWD of PE.     

Oxygen-copper (II) interplay in the repair of semi-oxidized urate by quercetin bound to human serum albumin

The 1:1 complex of copper (II) and human serum albumin (HSA) slowly reacts with radiolytically generated ^•O₂^- radical-anion at a rate constant of 6.1×10₆ M_-1 s_-1. Absorbance and fluorescence spectroscopies demonstrate that addition of an equimolar portion of quercetin (QH₂) to the solution of the copper (II)-HSA complex induces a relocalization of the copper resulting in a ternary copper (II)-QH₂-HSA complex. This form of quercetin slowly oxidizes in air-saturated solutions. A 10-fold excess urate, a plasma antioxidant, cannot displace copper (II) bound to HSA. In N₂O-saturated solutions the ternary complex form of QH₂ can repair the urate radical with a rate constant of 2.7×10₆ M_-1 s_-1 by an electron transfer reaction similar to that observed in the absence of copper (II). In O₂-saturated solutions and in the absence of copper, HSA-bound QH₂ fails to repair the urate radical because of the fast competitive reaction of ^•O₂^- with urate radicals. However, addition of equimolar copper (II) restores the electron transfer from QH₂ to the urate radical. These contrasting results are tentatively explained either by an enhanced reactivity of copper (II) with ^•O₂^- in the ternary complex or by direct production of quercetin radicals via a copper-catalyzed reduction of the ^•O₂^- radicals by QH₂.     

Functional reconstitution of G-protein-coupled receptor-mediated adenylyl cyclase activation by a baculoviral co-display system

Recently, evidence has accumulated in support of the heterologous expression of functional membrane proteins and their complexes on extracellular baculovirus particles (budded virus, BV). In this study, we attempted to apply this BV display system to detect G-protein-coupled receptor (GPCR) signaling. We infected Sf9 cells with a combination of four recombinant baculoviruses individually encoding the dopamine D1 receptor (DR-D1), G-protein -subunit (G_s), G-protein β₁γ₂ subunit dimer (Gβ₁γ₂), and adenylyl cyclase type VI (ACVI). The recovered BV fraction produced cAMP in response to the stimulation with dopamine. Co-expression of all three G-protein subunits in addition to receptor and ACVI led to a maximal response. BV co-expressing DR-D1, G_s, Gβ₁γ₂, and ACVI also responded to dopamine agonists and an antagonist. Furthermore, BV expressing two other G_s-coupled receptors together with G_s, Gβ₁γ₂, and ACVI also produced cAMP in response to their specific ligands. These results indicate the functional coupling of receptor, G_s and ACVI is reconstituted on BV. Since BV is essentially free of endogenous GPCRs, this BV co-display system should prove highly useful for the development of functional assay systems for GPCRs.     

Electron and light microscopy of neutrophil responses in mice vaccinated and challenged with third-stage infective hookworm (Ancylostoma caninum) larvae.

The role of neutrophils in mediating host inflammation was examined in mice vaccinated with living third-stage infective hookworm larvae (L₃). Mice were vaccinated by oral immunization with 500 L₃ (Ancylostoma caninum) once every 2 weeks for a total of three immunizations. The vaccinated mice were then challenged intraperitoneally with 2000 L_3, 1 week after the final immunization. To stimulate peritoneal production of neutrophils, 2 ml of 2% glycogen were injected intraperitoneally at 16 h prior to the challenge infection. Neutrophils were found to comprise 85% of the peritoneal cell population. L₃ from the challenge infection were collected and then examined at timed intervals by inverted light microscopy, scanning electron microscopy (SEM) and transmission electron microscopy (TEM). Greater than a fivefold increase in the total numbers of peritoneal cells was noted in the vaccinated mice as compared to unvaccinated mice. In the peritoneal cavity of vaccinated mice, the neutrophils adhered to the L₃ within 2 h, and over 55% of the L₃ were surround by clusters of neutrophils to form a sausage-like sheath 4 h later. At 24–72 h after challenge, almost all of the L₃ recovered from the vaccinated mice were covered with thick clusters of cells. Both SEM and TEM demonstrated extensive ultrastructural damage to the L_3. In contrast, the L₃ recovered from the unvaccinated mice appeared to be unaffected by neutrophils. These studies suggest that neutrophils, like macrophages, can have an important role as effector cells in L₃-vaccinated mice.     

Reactions between ruthenium cluster carbonyls and 1,4-diphenylbuta-1,3-diyne

The complexes RuC(CCPh)=CPhC(CCPh)=CPh(CO)₃(NMe₃) (3), Ru₂μ-C(CCPh)=CPhC(CCPh)=CPh(CO)₆ (1), Ru₂μ-[C(CCPh)=CPh]₂CO(CO)₆ (2), Ru₃(μ₃-PhC₂CCPh)(μ-CO)(CO)₉ (4) and Ru₄(μ₄-PhC₂CCPh)(CO)₁₂ (5) have been isolated from reactions between PhC₂C₂Ph and Ru₃(CO)₁₂ or RU₃(CO)₁₀(NCMe)₂. The molecular structures of complexes 1, 2, 3 and 5 have been determined from single-crystal X-ray studies. All complexes have precedents in similar products obtained from reactions involving mono-ynes; in the present cases, each alkyne fragment retains a phenylethynyl (PhCC---) group as a non-coordinated substituent.     

Synthesis and characterization of disubstituted arylcyanoximes and their several metal complexes

A series of new disubstituted halogenated arylcyanoximes was synthesized using nitrosation reaction of the respective phenylacetonitriles by CH₃–ONO at room temperature in isopropanol. Six synthesized colorless arylcyanoximes containing two F and/or Cl atoms at 2-, 4-, 5- and 6-positions were characterized by means of NMR, IR, UV–Vis spectroscopy and pK_a studies. Crystal structures were determined for four cyanoximes and revealed the presence of only the syn-isomers for fluorinated compounds in a solid state, while the chlorinated arylcyanoxime exists as anti-isomer in the crystal. However, five out of the six protonated arylcyanoximes HL exist as a mixture of syn- and anti-isomers in solutions. Deprotonation of HL with NaOC₂H₅ in ether solutions leads to yellow NaL which were used as precursors for the synthesis of a series of monovalent Ag, Tl and bivalent Pd, Pt complexes. Seven palladium and platinum arylcyanoximates of [M(HL)₂Cl₂] composition were synthesized and characterized. Obtained colored compounds are non-electrolytes in solution. However, in EtOH and DMSO solutions Pt(II) cyanoximates undergo two consecutive solvolysis reactions. First order rate constants were measured at 294 K for complexes in both solvents. Binding modes of the cyanoxime ligands and the possible solid state structures of the obtained coordination compounds are suggested on a basis of their IR spectra and MM-2 calculations. Because of their structural resemblance to the cisplatin family of anticancer drugs, synthesized Pd/Pt arylcyanoximates were tested in vitro against human colon carcinoma WiDr cell line using cis-[Pt(NH₃)₂Cl₂] as positive control. Results showed that two Pd(II) and Pt(II) cyanoximates containing oximino(2,4-dichlorophenyl)acetonitrile exhibit cytotoxicity at 0.25 mM concentrations.     

不同施氮水平下杨树-苋菜间作系统对土壤氮素流失的影响

采用田间试验方法,研究了杨树 苋菜间作系统,即株行距2 m×5 m(L₁)和2 m×15 m(L₂)在0(N₀)、91(N₁)、137(N₂)和183(N₃) kg·hm^-2施氮水平下的土壤氮素流失特征.结果表明: 不同施氮水平对地表径流量、淋溶量和土壤侵蚀量的控制效果均为L₁＞L₂＞L₃ (单作苋菜);L₁、L₂地表径流量分别比L₃降低65.1%、55.9%;L₁、L₂距林带0.5 m处淋溶量比L₃降低30.0%、28.9%,距林带1.5 m处淋溶量比L₃降低25.6%、21.9%;L₁、L₂土壤侵蚀量分别比L₃降低65.0%、55.1%.对地表径流和淋溶损失中TN、NO₃^--N、NH₄⁺-N流失量的控制效果均为L₁＞L₂＞L₃;常规施氮(91 kg·hm^-2)水平下,L₁地表径流中TN、NO₃^--N、NH₄⁺-N流失量较L₃分别降低62.9%、45.1%、69.2%,L₂较L₃分别降低23.4%、6.9%、46.2%;杨树间作密度越大、距离林带越近,对土壤NO₃^--N、NH₄⁺-N的淋溶损失削减作用越强.同一间作密度下,随着施氮量的增加,地表径流中NO₃^--N流失比例减少,NH₄⁺-N流失比例增加;淋溶流失中
NO₃^--N、NH₄⁺-N浓度变化趋势一致,均为 N₃＞N₂＞N₁＞N₀.     

Syntheses and properties of organocyanamide, cyanoguanidine and dinitrogen complexes of rhenium. Crystal structure of mer-[ReCl2(NCNEt2) (PMePh2)3]

Treatment of a THF solution of trans-[ReCl(N₂)L₄] (L = PMePh₂) with a cyanamide, NCNR₂ (R = Me, Et or H) or with cyanoguanidine, NCNC(NH₂)₂ , yields mer-[ReCl(N₂)(NCNR₂)L₃] (1) or mer-[Re(N₂)[Re(N₂){NCNC(NH₂)₂}₂L₃]Cl (2), respectively, which, to our knowledge, are the first mixed dinitrogen-cyanamide-type complexes to be reported. The former products (1, R=Me or Et) can also be obtained from reaction of the benzoyldiazenido complex [ReCl₂(NNCOPh)L₃] with NCNR₂ in refluxing methanol; the Re(II) complex mer-[ReCl₂(NCNEt₂)L₃] (3) is also formed (conceivably via an unusual homolysis of the C---N bond of the benzoyldiazenido ligand) and its crystal structure is reported. It shows an unusual pyramidal conformation at the amine N atom of the diethylcyanamide ligand which also exhibits a significant structural trans influence on the phosphine, behaving as a stronger net electron donor than the latter ligand.     

Synthesis, growth inhibition, and cell cycle evaluations of novel flavonoid derivatives

As a continuation of our search for potential new anticancer agents, a series of ten flavonoid derivatives has been synthesized by cyclization of substituted chalcones. Target compounds were evaluated for their biological activity. Among them, compounds 1–4 and 9 displayed a significant growth inhibitory action against a panel of tumor cell lines including Jurkat, PC-3, and Colon 205. On treatment with an equitoxic (IC₅₀) concentration, compounds 1–5 and 7–9 blocked cells in the G2/M phase of the Jurkat cell cycle, whereas compound 6 blocked the same in the G0/G1 phase.     

Synthesis and histamine H3 receptor activity of 4-(n-alkyl)-1H-imidazoles and 4-(omega-phenylalkyl)-1H-imidazoles

The influence of lipophilic moieties attached to a 4-1H-imidazole ring on the histamine H₃ receptor activity was systematically investigated. Series of 4-(n-alkyl)-1H-imidazoles and 4-(ω-phenylalkyl)-1H-imidazoles were prepared, with an alkyl chain varying from 2–9 methylene groups and from 1–9 methylene groups, respectively. The compounds were tested for their activity on the H₃ receptor under in vitro conditions. For the 4-(n-alkyl)-1H-imidazoles the activity is proportional to chain length, ranging from a pA₂ value of 6.3±0.2 for 4-(n-propyl)-1H-imidazole to a pA₂ value of 7.2±0.1 for 4-(n-decyl)-1H-imidazole. For the series 4-(ω-phenylalkyl)-4H-imidazoles an optimum in H₃ activity was found for the pentylene spacer: 4-(ω-phenylpentyl)-1H-imidazole has a pA₂ value of 7.8±0.1.