• 약학회지
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• 제50권2호
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• pp.93-98
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• 2006

Human foamy virus (HFV) integrase mediates integration of viral c-DNA into cellular DNA. In this process, HFV prointegration complex (PIC) in which integrase is a key component moves to nuclei of the infected cells and leads to integration of viral DNA to the cellular genome, which is essential in viral life cycle. In general nuclear localization signals (NLS) have been suggested to be involved in localizing retroviral PIC to nuclei, but the mechanisms for nuclear localization of the HFV PIC remains unclear. To functionally identify the NLS of HFV integrase, various subdomains of the protein were expressed as GFP fusions and their subcellular locations were analyzed with confocal laser scanning microscopy. Wild type HFV integrase was karyophilic by targeting the fusion protein to nuclei of the COS-1 and 293T cells. Our results showed that strong NLS of HFV integrase was mapped to the C-terminal regions. In addition the karyophilic properties of N-terminal and central regions are not individually strong enough to direct localization of the fusion proteins to nuclei, but their cooperative activity for nuclear import was confirmed.

• Molecules and Cells
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• 제27권3호
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• pp.359-363
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• 2009

Chfr, a checkpoint with FHA and RING finger domains, plays an important role in cell cycle progression and tumor suppression. Chfr possesses the E3 ubiquitin ligase activity and stimulates the formation of polyubiquitin chains by Ub-conjugating enzymes, and induces the proteasome-dependent degradation of a number of cellular proteins, including Plk1 and Aurora A. While Chfr is a nuclear protein that functions within the cell nucleus, how Chfr is localized in the nucleus has not been clearly demonstrated. Here, we show that nuclear localization of Chfr is mediated by nuclear localization signal (NLS) sequences. To reveal the signal sequences responsible for nuclear localization, a short lysine-rich stretch (KKK) at amino acid residues 257-259 was replaced with alanine, which completely abolished nuclear localization. Moreover, we show that nuclear localization of Chfr is essential for its checkpoint function but not for its stability. Thus, our results suggest that NLS-mediated nuclear localization of Chfr leads to its accumulation within the nucleus, which may be important in the regulation of Chfr activation and Chfr-mediated cellular processes, including cell cycle progression and tumor suppression.

• 한국군사과학기술학회지
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• 제14권4호
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• pp.590-597
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• 2011

The IDRS provides detection, classification and bearing/range estimation by performing wavefront curvature analysis on an intercepted active transmission from target. Especially, a estimate of the target bearing/range that significantly affects the optimal operation of own submarine is required. Target bearing/range can be estimated by wavefront curvature ranging which use the difference of time arrival at sensors. But estimation ambiguity occur in bearing/range estimation due to a number of peaks caused by high center frequency and limited bandwidth of the intercepted active transmission and distortion caused by noise. As a result the bearing/range estimation performance is degraded. To estimate target bearing/range correctly, bearing/range estimation method that eliminate estimation ambiguity is required. In this paper, therefore, for wavefront curvature ranging, NLS cost function with curve fitting method is proposed, which provide robust bearing/range estimation performance by eliminating estimation ambiguity. Through simulation the performance of the proposed bearing/range estimation methods are verified.

• 한국통신학회논문지
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• 제27권8A호
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• pp.814-821
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• 2002

SPIHT(set partitioning in hierarchical tree)는 제로트리 알고리즘 중 효율적이며 잘 알려져 있다. 그러나 높은 메모리 요구로 인해 하드웨어 구현에 큰 어려움을 가지고 있다. 본 논문에서는 저 메모리 사용과 빠른 제로트리 부호화 알고리즘을 제안한다. 메모리를 줄이고 빠른 코딩을 위한 방법으로 다음 3가지를 제안한다. 첫 번째, 리프팅(lifting)을 이용한 웨이블릿(wavelet) 변환은 기존의 필터뱅크 방식의 변환보다 저 메모리와 계산량의 감소를 가진다. 두 번째 방법은 웨이블릿 계수들을 블록으로 나누어 각각 부호화 한다. 여기서 블록은 제로트리 구조가 유지되는 STB(spatial tree-based block)이다. 마지막으로 Wheeler와 Pearlmandl 제안한 NLS(no list SPIHT)를 이용한 부호화이다. NLS의 효율성은 SPIHT와 거의 같으며 작고 고정된 메모리와 빠른 부호화 속도를 보여준다.

• Nuclear Medicine and Molecular Imaging
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• 제41권4호
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• pp.317-325
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• 2007

동적 PET 데이터는 구획모델과 Nonlinear Least Squares(NLS)방법을 사용하여 분석함으로서 각종 생화학적 물질의 생체 대사율 등을 정량화 할 수 있다. 하지만 NLS방법은 변수의 초기 값이 적절하지 않을 경우 지역적인 최소점에 빠지거나 계산시간이 길어 동역학 변수들을 각 화소마다 구해야 하는 파라메터 영상(parametric image) 구성에는 효과적이지 않다. Patlak 도표분석법(PGA)은 비선형 방정식을 선형화하여 값을 추정함으로서 간단하면서 적은 계산량으로 인해 파라메터 영상을 구성하는데 많이 사용되고 있으나 잡음성분과 선형구간 선정에 따라 값이 영향을 받는 단점이 있다. 따라서 이 연구에서는 3구획 비가역 모델에 적합한 다중선형분석법(MLAIR)을 고안하였으며 3구획 비가역 모델의 대표적 예인 $[^{18}F]Fluoride$ PET을 이용하여 미니돼지에서의 뼈 섭취률을 계산하여 PGA방법과 비교 분석해 보았다. 대상 및 방법: 3마리의 미니돼지를 대상으로 100MBq의 $[^{18}F]Fluoride$를 대퇴부 정맥에 주사하면서 ECAT EXAET 47 PET 스캐너를 이용하여 60분간 PET 영상을 얻었다. 케타민과 자일라진을 이용하여 30분 간격으로 마취하였으며 실험동물을 진공 쿠션을 이용하여 반드시 누운 자세로 위치하도록 고정 시켰다. 입력함수인 혈장 내 농도곡선은 대퇴동맥으로부터 스캔 시작과 함께 혈액 채취를 통해 얻었다. ROI분석을 위해 대퇴골두, 척추 뼈, 근육에 ROI를 그려 조직 내 시간-방사능 곡선을 얻었다. $k_4$가 0인 3구획 비가역 모델로부터 MLAIR와 PGA방법을 사용하여 관심영역에서의 뼈 섭취률 $K_i$와 파라메터 영상을 구성하였다. PGA방법은 선형구간의 시작점인 $t^*$선택에 따른 영향을 보기 위해 분석구간을 변화시켜가며 분석하였다. 결과: ROI 분석결과 추정된 $K_i$값은 NLS방법에 비하여 MLAIR방법과 PGA방법 모두에서 과대 추정되었으나 두 분석방법 끼리는 비슷한결과를 보였다. Patlak 기울기는 $t^*$선택에 따라 값이 변하였으며 Patlak 상수는 Fluoride 섭취가 높은 대퇴골두나 척추뼈에서 30분이 지나서야 일정한 값으로 나타났고 섭취가 낮은 근육에서는 10분만에 일정해졌다. 파라메터 영상에서는 제안한 MLAIR방법이 PGA방법에 비해 영상의 질을 향상시킴을 알 수 있었다. 또한 PGA방법을 이용하여 구성한 파라메터 영상은 $t^*$값이 커질수록 급격히 영상의 질이 저하됨을 볼 수 있다. 특히 Fluoride 섭취가 높은 영역에서 Patlak 상수가 일정해지는 시간인 $t^*$값이 30분일 때 파라메터 영상은 MLAIR와 크게 차이가 났다. 결론 결론적으로 제안한 MLAIR방법은 선형구간을 정할 필요 없이 모든 데이터를 사용하는 이점이 있으며 선형적인 방법을 통해 $K_i$값을 얻을 수 있어 계산시간을 단축 시켜 줄 뿐 아니라 잡음성분에 강해 파라메터 영상의 질을 크게 향상 시켜 줌으로 비가역 3구획모델에서의 PGA방법을 대체할 새로운 파라메터 영상구성방법으로 적합할 것이다.

• Journal of Communications and Networks
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• 제5권4호
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• pp.303-308
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• 2003

We present a statistical model for the path loss of ultrawideband (UWB) channels in indoor environments. In contrast to our previously reported measurements, the data reported here are for a bandwidth of 6GHz rather than 1.25GHz; they encompass commercial buildings in addition to single-family homes (20 of each); and local spatial averaging is included. As before, the center frequency is 5.0GHz. Separate models are given for commercial and residential environments and, within each category, for lineof sight (LOS) and non-line-of-sight (NLS) paths. All four models have the same mathematical structure, differing only in their numerical parameters. The two new models (LOS and NLS) for residences closely match those derived from the previous measurements, thus affirming the stability of our path loss modeling. We find, also, that the path loss statistics for the two categories of buildings are quite similar.

• 한국경영과학회지
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• 제38권1호
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• pp.45-59
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• 2013

A long-term forecasting method for a new product in early stage of diffusion is proposed. The method includes a constrained non-linear least square estimation with the logistic diffusion model. The constraints would be critical market informations such as market potential, peak point, and take-off. Findings on 20 cases having almost full life cycle are that (i) combining any market information improves the forecasting accuracy, (ii) market potential is the most stable information, and (iii) peak point and take-off information have negative effect in case of overestimation.

• Mycobiology
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• 제50권5호
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• pp.259-268
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• 2022

The nuclear import of proteins is a fundamental process in the eukaryotes including plant. It has become evident that such basic process is exploited by nuclear effectors that contain nuclear localization signal (NLS) and are secreted into host cells by fungal pathogens of plants. However, only a handful of nuclear effectors have been known and characterized to date. Here, we first summarize the types of NLSs and prediction tools available, and then delineate examples of fungal nuclear effectors and their roles in pathogenesis. Based on the knowledge on NLSs and what has been gleaned from the known nuclear effectors, we point out the gaps in our understanding of fungal nuclear effectors that need to be filled in the future researches.

• 한국양식학회:학술대회논문집
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• 한국양식학회 2006년도 수산관련학회 공동학술대회 발표요지집
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• pp.491-493
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• 2006

• Journal of Microbiology and Biotechnology
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• 제30권1호
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• pp.109-117
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• 2020

Cre recombinase is widely used to manipulate DNA sequences for both in vitro and in vivo research. Attachment of a trans-activator of transcription (TAT) sequence to Cre allows TAT-Cre to penetrate the cell membrane, and the addition of a nuclear localization signal (NLS) helps the enzyme to translocate into the nucleus. Since the yield of recombinant TAT-Cre is limited by formation of inclusion bodies, we hypothesized that the positively charged arginine-rich TAT sequence causes the inclusion body formation, whereas its neutralization by the addition of a negatively charged sequence improves solubility of the protein. To prove this, we neutralized the positively charged TAT sequence by proximally attaching a negatively charged poly-glutamate (E12) sequence. We found that the E12 tag improved the solubility and yield of E12-TAT-NLS-Cre (E12-TAT-Cre) compared with those of TAT-NLS-Cre (TAT-Cre) when expressed in E. coli. Furthermore, the growth of cells expressing E12-TAT-Cre was increased compared with that of the cells expressing TAT-Cre. Efficacy of the purified TAT-Cre was confirmed by a recombination test on a floxed plasmid in a cell-free system and 293 FT cells. Taken together, our results suggest that attachment of the E12 sequence to TAT-Cre improves its solubility during expression in E. coli (possibly by neutralizing the ionic-charge effects of the TAT sequence) and consequently increases the yield. This method can be applied to the production of transducible proteins for research and therapeutic purposes.